Discovery of 3,5-Dimethyl-4-Sulfonyl-1H-Pyrrole-Based Myeloid Cell Leukemia 1 Inhibitors with High Affinity, Selectivity, and Oral Bioavailability
发现具有高亲和性、选择性和口服生物利用度的 3,5-二甲基-4-磺酰基-1H-吡咯髓系细胞白血病 1 抑制剂

This article references 79 other publications.

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   Mitochondria and apoptosis

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   A review with 57 refs. A variety of key events in apoptosis focus on mitochondria, including the release of caspase activators (such as cytochrome c), changes in electron transport, loss of mitochondrial transmembrane potential, altered cellular oxidn.-redn., and participation of pro- and antiapoptotic Bcl-2 family proteins. The different signals that converge on mitochondria to trigger or inhibit these events and their downstream effects delineate several major pathways in physiol. cell death.

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   The Bcl-2 protein family: arbiters of cell survival

   Adams, Jerry M.; Cory, Suzanne

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   A review, with 61 refs. Bcl-2 and related cytoplasmic proteins are key regulators of apoptosis, the cell suicide program crit. for development, tissue homeostasis, and protection against pathogens. Those most similar to Bcl-2 promote cell survival by inhibiting adapters needed for activation of the proteases (Caspases) that dismantle the cell. More distant relatives instead promote apoptosis, apparently through mechanisms that include displacing the adapters from the pro-survival proteins. Thus, for many but not all apoptotic signals, the balance between these competing activities dets. cell fate. Bcl-2 family members are essential for maintenance of major organ systems, and mutations affecting them are implicated in cancer.

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   Lutz, R. J. Role of the BH3 (Bcl-2 homology 3) domain in the regulation of apoptosis and Bcl-2-related proteins. Biochem. Soc. Trans. 2000, 28, 51– 56,  DOI: 10.1042/bst0280051

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   Role of the BH3 (Bcl-2 homology 3) domain in the regulation of apoptosis and Bcl-2-related proteins

   Lutz, R. J.

   Biochemical Society Transactions (2000), 28 (2), 51-55CODEN: BCSTB5; ISSN:0300-5127. (Portland Press Ltd.)

   A review, with 9 refs. The Bcl-2 family of proteins play a prominent role in the regulation of apoptosis. From the initial identification of bcl-2 as an oncogene in follicular lymphoma through genetic studies in Caenorhabditis elegans to recent functional studies focusing on the importance of mitochondrial events in cell death signaling, the members of this protein family continue to be implicated in pivotal decision points regarding the survival of the cell. The family can be divided into 2 classes: those such as Bcl-2 and Bcl-xL that suppress cell death, and others, such as Bak and Bax, that appear to promote apoptosis. The Bcl-2 family is characterized by specific regions of homol. termed Bcl-2 homol. (BH1, BH2, BH3, and BH4) domains, which are crit. to the function of these proteins, including their impact on cell survival and their ability to interact with other family members and regulatory proteins. The identification of the BH3 domain as a potent mediator of cell death has led to the emergence of an addnl. family of proapoptotic proteins (such as Bad, Bik, Bid, and Hrk) that share identity with Bcl-2 only within this death domain. These BH3-only proteins may be part of a regulatory network serving to integrate cell survival and death signals, an assertion that is supported by the identification of a BH3-only protein, Egl-1, as part of the central core of cell death signaling in C. elegans. While the mechanism of action of the BH3-only proteins remains unclear, recent studies on the regulation of crit. protein-protein interactions and activity of Bad by phosphorylation in response to growth factor signaling suggest that the active state of BH3-only proteins may be regulated by post-translational modification. Addnl. modes of regulation, such as transcriptional, translational, and subcellular localization, are also likely to be important.

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   Ren, D.; Tu, H.-C.; Kim, H.; Wang, G. X.; Bean, G. R.; Takeuchi, O.; Jeffers, J. R.; Zambetti, G. P.; Hsieh, J. J.-D.; Cheng, E. H.-Y. BID, BIM, and PUMA are essential for activation of the BAX- and BAK-dependent cell death program. Science 2010, 330, 1390– 1393,  DOI: 10.1126/science.1190217

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   BID, BIM, and PUMA Are Essential for Activation of the BAX- and BAK-Dependent Cell Death Program

   Ren, Decheng; Tu, Ho-Chou; Kim, Hyungjin; Wang, Gary X.; Bean, Gregory R.; Takeuchi, Osamu; Jeffers, John R.; Zambetti, Gerard P.; Hsieh, James J.-D.; Cheng, Emily H.-Y.

   Science (Washington, DC, United States) (2010), 330 (6009), 1390-1393CODEN: SCIEAS; ISSN:0036-8075. (American Association for the Advancement of Science)

   Although the proteins BAX and BAK are required for initiation of apoptosis at the mitochondria, how BAX and BAK are activated remains unsettled. We provide in vivo evidence demonstrating an essential role of the proteins BID, BIM, and PUMA in activating BAX and BAK. Bid, Bim, and Puma triple-knockout mice showed the same developmental defects that are assocd. with deficiency of Bax and Bak, including persistent interdigital webs and imperforate vaginas. Genetic deletion of Bid, Bim, and Puma prevented the homo-oligomerization of BAX and BAK, and thereby cytochrome c-mediated activation of caspases in response to diverse death signals in neurons and T lymphocytes, despite the presence of other BH3-only mols. Thus, many forms of apoptosis require direct activation of BAX and BAK at the mitochondria by a member of the BID, BIM, or PUMA family of proteins.

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   The release of cytochrome c from mitochondria: a primary site for Bcl-2 regulation of apoptosis

   Kluck, Ruth M.; Bossy-Wetzel, Ella; Green, Douglas R.; Newmeyer, Donald D.

   Science (Washington, D. C.) (1997), 275 (5303), 1132-1136CODEN: SCIEAS; ISSN:0036-8075. (American Association for the Advancement of Science)

   In a cell-free apoptosis system, mitochondria spontaneously released cytochrome c, which activated DEVD-specific caspases, leading to fodrin cleavage and apoptotic nuclear morphol. Bcl-2 acted in situ on mitochondria to prevent the release of cytochrome c and thus caspase activation. During apoptosis in intact cells, cytochrome c translocation was similarly blocked by Bcl-2 but not by a caspase inhibitor, zVAD-fmk. In vitro, exogenous cytochrome c bypassed the inhibitory effect of Bcl-2. Cytochrome c release was unaccompanied by changes in mitochondrial membrane potential. Thus, Bcl-2 acts to inhibit cytochrome c translocation, thereby blocking caspase activation and the apoptotic process.

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   Kozopas, K. M.; Yang, T.; Buchan, H. L.; Zhou, P.; Craig, R. W. Mcl-1, a gene expressed in programmed myeloid cell differentiation, has sequence similarity to Bcl-2. Proc. Natl. Acad. Sci. U. S. A. 1993, 90, 3516– 3520,  DOI: 10.1073/pnas.90.8.3516

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   MCL1, a gene expressed in programmed myeloid cell differentiation, has sequence similarity to BCL2

   Kozopas, Karen M.; Yang, Tao; Buchan, Heather L.; Zhou, Ping; Craig, Ruth W.

   Proceedings of the National Academy of Sciences of the United States of America (1993), 90 (8), 3516-20CODEN: PNASA6; ISSN:0027-8424.

   A gene, MCL1, was isolated from the ML-1 human myeloid leukemia cell line during phorbol ester-induced differentiation along the monocyte/macrophage pathway. Expression of MCL1 increases early in the induction, or programming, of differentiation in ML-1 (at 1-3 h), before the appearance of differentiation markers and mature morphol. (at 1-3 days). Further, MCL1 has sequence similarity to BCL2, a gene involved in normal lymphoid development and in lymphomas with the t(14;18) chromosome translocation. MCL1 and BCL2 do not fall into previously known gene families. BCL2 differs from many oncogenes in that it inhibits programmed cell death, promoting viability rather than proliferation; this parallels the assocn. of MCL1 with the programming of differentiation and concomitant maintenance of viability but not proliferation. Thus, in contrast to proliferation-assocd. genes, expression of MCL1 and BCL2 relates to the programming of differentiation and cell viability/death.

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   Herrant, M.; Jacquel, A.; Marchetti, S.; Belhacène, N.; Colosetti, P.; Luciano, F.; Auberger, P. Cleavage of Mcl-1 by caspases impaired its ability to counteract Bim-induced apoptosis. Oncogene 2004, 23, 7863– 7873,  DOI: 10.1038/sj.onc.1208069

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   Cleavage of Mcl-1 by caspases impaired its ability to counteract Bim-induced apoptosis

   Herrant, Magali; Jacquel, Arnaud; Marchetti, Sandrine; Belhacene, Nathalie; Colosetti, Pascal; Luciano, Frederic; Auberger, Patrick

   Oncogene (2004), 23 (47), 7863-7873CODEN: ONCNES; ISSN:0950-9232. (Nature Publishing Group)

   Mcl-1 is an antiapoptotic member of the Bcl-2 family that can promote cell viability. We report here that Mcl-1 is a new substrate for caspases during induction of apoptosis. Mcl-1 cleavage occurs after Asp127 and Asp157 and generates four fragments of 24, 19, 17 and 12 kDa in both intact cells and in vitro, an effect prevented by selective caspase inhibitors. As a consequence, the resulting protein that lacks the first 127 or 157 amino acids contains only the BH1-BH3 domains of Bcl-2 family members. Mutation of Asp127 and Asp157 abolishes the generation of the 24 and 12 kDa fragments and that of the 19 and 17 kDa fragments, resp. Interestingly, when expressed in HeLa cells Mcl-1 wt and Mcl-1 Δ127 showed a markedly different intracellular distribution. Mcl-1 wt colocalized with α-Tubulin near the internal face of the plasma membrane, while Mcl-1 Δ127 co-assocd. with Bim-EL at the mitochondrial level. Coimmunopptn. expts. also demonstrated that Mcl1 Δ127 exhibited increased binding to Bim when compared to Mcl-1 wt. Finally, Mcl-1 wt unlike Mcl-1 Δ127 inhibited Bim-EL-induced caspase activation. Altogether, our findings demonstrate that cleavage of Mcl-1 by caspases modifies its subcellular localization, increases its assocn. with Bim and inhibits its antiapoptotic function.

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8. 8

   Adams, J. M.; Cory, S. Life-or-death decisions by the Bcl-2 protein family. Trends Biochem. Sci. 2001, 26, 61– 66,  DOI: 10.1016/S0968-0004(00)01740-0

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   Life-or-death decisions by the Bcl-2 protein family

   Adams, J. M.; Cory, S.

   Trends in Biochemical Sciences (2001), 26 (1), 61-66CODEN: TBSCDB; ISSN:0968-0004. (Elsevier Science Ltd.)

   A review, with 51 refs. In response to intracellular damage and certain physiol. cues, cells enter the suicide program termed apoptosis, executed by proteases called caspases. Commitment to apoptosis is typically governed by opposing factions of the Bcl-2 family of cytoplasmic proteins. Initiation of the proteolytic cascade requires assembly of certain caspase precursors on a scaffold protein, and the Bcl-2 family dets. whether this complex can form. Its pro-survival members can act by sequestering the scaffold protein and/or by preventing the release of apoptogenic mols. from organelles such as mitochondria. Pro-apoptotic family members act as sentinels for cellular damage: cytotoxic signals induce their translocation to the organelles where they bind to their pro-survival relatives, promote organelle damage and trigger apoptosis.

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9. 9

   Gomez-Bougie, P.; Wuillème-Toumi, S.; Ménoret, E.; Trichet, V.; Robillard, N.; Philippe, M.; Bataille, R.; Amiot, M. Noxa up-regulation and Mcl-1 cleavage are associated to apoptosis induction by bortezomib in multiple myeloma. Cancer Res. 2007, 67, 5418– 5424,  DOI: 10.1158/0008-5472.CAN-06-4322

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   Noxa Up-regulation and Mcl-1 Cleavage Are Associated to Apoptosis Induction by Bortezomib in Multiple Myeloma

   Gomez-Bougie, Patricia; Wuilleme-Toumi, Soraya; Menoret, Emmanuelle; Trichet, Valerie; Robillard, Nelly; Philippe, Moreau; Bataille, Regis; Amiot, Martine

   Cancer Research (2007), 67 (11), 5418-5424CODEN: CNREA8; ISSN:0008-5472. (American Association for Cancer Research)

   Targeting the ubiquitin-proteasome pathway has emerged as a potent anticancer strategy. Bortezomib, a specific proteasome inhibitor, has been approved for the treatment of relapsed or refractory multiple myeloma. Multiple myeloma cell survival is highly dependent on Mcl-1 antiapoptotic mols. In a recent study, proteasome inhibitors induced Mcl-1 accumulation that slowed down their proapoptotic effects. Consequently, we investigated the role of Bcl-2 family members in bortezomib-induced apoptosis. We found that bortezomib induced apoptosis in five of seven human myeloma cell lines (HMCL). Bortezomib-induced apoptosis was assocd. with Mcl-1 cleavage regardless of Mcl-1L accumulation. Furthermore, RNA interference mediated Mcl-1 decrease and sensitized RPMI-8226 HMCL to bortezomib, highlighting the contribution of Mcl-1 in bortezomib-induced apoptosis. Interestingly, an important induction of Noxa was found in all sensitive HMCL both at protein and mRNA level. Concomitant to Mcl-1 cleavage and Noxa induction, we also found caspase-3, caspase-8, and caspase-9 activation. Under bortezomib treatment, Mcl-1L/Noxa complexes were highly increased, Mcl-1/Bak complexes were disrupted, and there was an accumulation of free Noxa. Finally, we obsd. a dissocn. of Mcl-1/Bim complexes that may be due to a displacement of Bim induced by Noxa. Thus, in myeloma cells, the mechanistic basis for bortezomib sensitivity can be explained mainly by the model in which the sensitizer Noxa can displace Bim, a BH3-only activator, from Mcl-1, thus leading to Bax/Bak activation.

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10. 10

    Pierson, W.; Cauwe, B.; Policheni, A.; Schlenner, S. M.; Franckaert, D.; Berges, J.; Humblet-Baron, S.; Schönefeldt, S.; Herold, M. J.; Hildeman, D.; Strasser, A.; Bouillet, P.; Lu, L.-F.; Matthys, P.; Freitas, A. A.; Luther, R. J.; Weaver, C. T.; Dooley, J.; Gray, D. H.; Liston, A. Antiapoptotic Mcl-1 is critical for the survival and niche-filling capacity of Foxp3⁺ regulatory T cells. Nat. Immunol. 2013, 14, 959– 965,  DOI: 10.1038/ni.2649

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    10

    Antiapoptotic Mcl-1 is critical for the survival and niche-filling capacity of Foxp3+ regulatory T cells

    Pierson, Wim; Cauwe, Benedicte; Policheni, Antonia; Schlenner, Susan M.; Franckaert, Dean; Berges, Julien; Humblet-Baron, Stephanie; Schoenefeldt, Susann; Herold, Marco J.; Hildeman, David; Strasser, Andreas; Bouillet, Philippe; Lu, Li-Fan; Matthys, Patrick; Freitas, Antonio A.; Luther, Rita J.; Weaver, Casey T.; Dooley, James; Gray, Daniel H. D.; Liston, Adrian

    Nature Immunology (2013), 14 (9), 959-965CODEN: NIAMCZ; ISSN:1529-2908. (Nature Publishing Group)

    Foxp3+ regulatory T (Treg) cells are a crucial immunosuppressive population of CD4+ T cells, yet the homeostatic processes and survival programs that maintain the Treg cell pool are poorly understood. Here we report that peripheral Treg cells markedly alter their proliferative and apoptotic rates to rapidly restore numerical deficit through an interleukin 2-dependent and costimulation-dependent process. By contrast, excess Treg cells are removed by attrition, dependent on the Bim-initiated Bak- and Bax-dependent intrinsic apoptotic pathway. The antiapoptotic proteins Bcl-xL and Bcl-2 were dispensable for survival of Treg cells, whereas Mcl-1 was crit. for survival of Treg cells, and the loss of this antiapoptotic protein caused fatal autoimmunity. Together, these data define the active processes by which Treg cells maintain homeostasis via crit. survival pathways.

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11. 11

    Renjini, A. P.; Titus, S.; Narayan, P.; Murali, M.; Jha, R. K.; Laloraya, M. STAT3 and MCL-1 associate to cause a mesenchymal epithelial transition. J. Cell Sci. 2014, 127, 1738– 1750,  DOI: 10.1242/jcs.138214

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    11

    STAT3 and MCL-1 associate to cause a mesenchymal epithelial transition

    Renjini, A. P.; Titus, Shiny; Narayan, Prashanth; Murali, Megha; Jha, Rajesh Kumar; Laloraya, Malini

    Journal of Cell Science (2014), 127 (8), 1738-1750CODEN: JNCSAI; ISSN:0021-9533. (Company of Biologists Ltd.)

    Embryo implantation is effected by a myriad of signaling cascades acting on the embryo-endometrium axis. Here we show, by using MALDI TOF anal., far-western anal. and colocalization and co-transfection studies, that STAT3 and MCL-1 are interacting partners during embryo implantation. We show in vitro that the interaction between the two endogenous proteins is strongly regulated by estrogen and progesterone. Implantation, pregnancy and embryogenesis are distinct from any other process in the body, with extensive, but controlled, proliferation, cell migration, apoptosis, cell invasion and differentiation. Cellular plasticity is vital during the early stages of development for morphogenesis and organ homeostasis, effecting the epithelial to mesenchymal transition (EMT) and, the reverse process, mesenchymal to epithelial transition (MET). STAT3 functionally assocs. with MCL-1 in the mammalian breast cancer cell line MCF7 that overexpresses STAT3 and MCL-1, which leads to an increased rate of apoptosis and decreased cellular invasion, disrupting the EMT. Assocn. of MCL-1 with STAT3 modulates the normal, anti-apoptotic, activity of MCL-1, resulting in pro-apoptotic effects. Studying the impact of the assocn. of STAT3 with MCL-1 on MET could lead to an enhanced understanding of pregnancy and infertility, and also metastatic tumors.

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12. 12

    Hikita, H.; Takehara, T.; Shimizu, S.; Kodama, T.; Li, W.; Miyagi, T.; Hosui, A.; Ishida, H.; Ohkawa, K.; Kanto, T.; Hiramatsu, N.; Yin, X. M.; Hennighausen, L.; Tatsumi, T.; Hayashi, N. Mcl-1 and Bcl-xL cooperatively maintain integrity of hepatocytes in developing and adult murine liver. Hepatology 2009, 50, 1217– 1226,  DOI: 10.1002/hep.23126

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    12

    Mcl-1 and Bcl-xL cooperatively maintain integrity of hepatocytes in developing and adult murine liver

    Hikita, Hayato; Takehara, Tetsuo; Shimizu, Satoshi; Kodama, Takahiro; Li, Wei; Miyagi, Takuya; Hosui, Atsushi; Ishida, Hisashi; Ohkawa, Kazuyoshi; Kanto, Tatsuya; Hiramatsu, Naoki; Yin, Xiao-Ming; Hennighausen, Lothar; Tatsumi, Tomohide; Hayashi, Norio

    Hepatology (Hoboken, NJ, United States) (2009), 50 (4), 1217-1226CODEN: HPTLD9; ISSN:0270-9139. (John Wiley & Sons, Inc.)

    Anti-apoptotic members of the Bcl-2 family, including Bcl-2, Bcl-xL, Mcl-1, Bcl-w and Bfl-1, inhibit the mitochondrial pathway of apoptosis. Bcl-xL and Mcl-1 are constitutively expressed in the liver. Although previous research established Bcl-xL as a crit. apoptosis antagonist in differentiated hepatocytes, the significance of Mcl-1 in the liver, esp. in conjunction with Bcl-xL, has not been clear. To examine this question, we generated hepatocyte-specific Mcl-1-deficient mice by crossing mcl-1flox/flox mice and AlbCre mice and further crossed them with bcl-xflox/flox mice, giving Mcl-1/Bcl-xL-deficient mice. The mcl-1flox/flox AlbCre mice showed spontaneous apoptosis of hepatocytes after birth, as evidenced by elevated levels of serum alanine aminotransferase (ALT) and caspase-3/7 activity and an increased no. of terminal deoxynucleotidyl transferase-mediated 2'-deoxyuridine 5'-triphosphate nick-end labeling (TUNEL)-pos. cells in the liver; these phenotypes were very dose to those previously found in hepatocyte-specific Bcl-xL-deficient mice. Although mcl-1flox/+ AlbCre mice did not display apoptosis, their susceptibility to Fas-mediated liver injury significantly increased. Further crossing of Mcl-1 mice with Bcl-xL mice showed that bcl-xflox/+ mcl-1flox/+ AlbCre mice also showed spontaneous hepatocyte apoptosis similar to Bcl-xL-deficient or Mcl-1-deficient mice. In contrast, bcl-xflox/flox mcl-1flox/+ AlbCre, bcl-xflox/+ mcl-1flox/flox AlbCre, and bcl-xflox/flox mcl-1flox/flox AlbCre mice displayed a decreased no. of hepatocytes and a reduced vol. of the liver on day 18.5 of embryogenesis and rapidly died within 1 day after birth, developing hepatic failure evidenced by increased levels of blood ammonia and bilirubin. Conclusion: Mcl-1 is crit. for blocking apoptosis in adult liver and, in the absence of Bcl-xL, is essential for normal liver development. Mcl-1 and Bcl-xL are two major anti-apoptotic Bcl-2 family proteins expressed in the liver and cooperatively control hepatic integrity during liver development and in adult liver homeostasis in a gene dose-dependent manner.

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13. 13

    Opferman, J. T.; Letai, A.; Beard, C.; Sorcinelli, M. D.; Ong, C. C.; Korsmeyer, S. J. Development and maintenance of B and T lymphocytes requires antiapoptotic MCL-1. Nature 2003, 426, 671– 676,  DOI: 10.1038/nature02067

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    13

    Development and maintenance of B and T lymphocytes requires antiapoptotic MCL-1

    Opferman, Joseph T.; Letai, Anthony; Beard, Caroline; Sorcinelli, Mia D.; Ong, Christy C.; Korsmeyer, Stanley J.

    Nature (London, United Kingdom) (2003), 426 (6967), 671-676CODEN: NATUAS; ISSN:0028-0836. (Nature Publishing Group)

    Regulated apoptosis is essential for both the development and the subsequent maintenance of the immune system. Interleukins, including IL-2, IL-4, IL-7 and IL-15, heavily influence lymphocyte survival during the vulnerable stages of VDJ rearrangement and later in ensuring cellular homeostasis, but the genes specifically responsible for the development and maintenance of lymphocytes have not been identified. The antiapoptotic protein MCL-1 is an attractive candidate, as it is highly regulated, appears to enhance short-term survival and functions at an apical step in genotoxic deaths. However, Mcl-1 deficiency results in peri-implantation lethality. Here we show that mice conditional for Mcl-1 display a profound redn. in B and T lymphocytes when MCL-1 is removed. Deletion of Mcl-1 during early lymphocyte differentiation increased apoptosis and arrested the development at pro-B-cell and double-neg. T-cell stages. Induced deletion of Mcl-1 in peripheral B- and T-cell populations resulted in their rapid loss. Moreover, IL-7 both induced and required MCL-1 to mediate lymphocyte survival. Thus, MCL-1, which selectively inhibits the proapoptotic protein BIM, is essential both early in lymphoid development and later on in the maintenance of mature lymphocytes.

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14. 14

    Thomas, L. W.; Lam, C.; Edwards, S. W. Mcl-1: the molecular regulation of protein function. FEBS Lett. 2010, 584, 2981– 2989,  DOI: 10.1016/j.febslet.2010.05.061

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    14

    Mcl-1; the molecular regulation of protein function

    Thomas, Luke W.; Lam, Connie; Edwards, Steven W.

    FEBS Letters (2010), 584 (14), 2981-2989CODEN: FEBLAL; ISSN:0014-5793. (Elsevier B.V.)

    A review. Apoptosis, an essential and basic biol. phenomenon, is regulated in a complex manner by a multitude of factors. Myeloid cell leukemia 1 (Mcl-1) protein, an anti-apoptotic member of the B-cell lymphoma 2 (Bcl-2) family of apoptosis-regulating proteins, exemplifies a no. of the mechanisms by which a protein's contribution to cell fate may be modified. The N-terminus of Mcl-1 is unique among the Bcl-2 family, in that it is rich in exptl. confirmed and putative regulatory residues and motifs. These include sites for ubiquitination, cleavage, and phosphorylation, which influence the protein's stability, localization, dimerization, and function. Here, the authors review what is known about the regulation of Mcl-1 expression and function, with particular focus on post-translational modifications and how phosphorylation interconnects the complex mol. control of Mcl-1 with the cellular state.

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15. 15

    Aichberger, K. J.; Mayerhofer, M.; Krauth, M. T.; Skvara, H.; Florian, S.; Sonneck, K.; Akgul, C.; Derdak, S.; Pickl, W. F.; Wacheck, V.; Selzer, E.; Monia, B. P.; Moriggl, R.; Valent, P.; Sillaber, C. Identification of Mcl-1 as a BCR/ABL-dependent target in chronic myeloid leukemia (CML): evidence for cooperative antileukemic effects of imatinib and mcl-1 antisense oligonucleotides. Blood 2005, 105, 3303– 3311,  DOI: 10.1182/blood-2004-02-0749

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    15

    Identification of mcl-1 as a BCR/ABL-dependent target in chronic myeloid leukemia (CML): Evidence for cooperative antileukemic effects of imatinib and mcl-1 antisense oligonucleotides

    Aichberger, Karl J.; Mayerhofer, Matthias; Krauth, Maria-Theresa; Skvara, Hans; Florian, Stefan; Sonneck, Karoline; Akgul, Cahit; Derdak, Sophia; Pickl, Winfried F.; Wacheck, Volker; Selzer, Edgar; Monia, Brett P.; Moriggl, Richard; Valent, Peter; Sillaber, Christian

    Blood (2005), 105 (8), 3303-3311CODEN: BLOOAW; ISSN:0006-4971. (American Society of Hematology)

    Antiapoptotic members of the bcl-2 family have recently been implicated in the pathogenesis of chronic myeloid leukemia (CML), a hematopoietic neoplasm assocd. with the BCR/ABL oncogene. The authors have examd. expression of MCL-1 in primary CML cells and BCR/ABL-transformed cell lines. Independent of the phase of disease, isolated primary CML cells expressed myeloid cell leukemia-1 (mcl-1) mRNA and the MCL-1 protein in a constitutive manner. The BCR/ABL inhibitor imatinib (=STI571) decreased the expression of MCL-1 in these cells. Correspondingly, BCR/ABL enhanced mcl-1 promoter activity, mcl-1 mRNA expression, and the MCL-1 protein in Ba/F3 cells. BCR/ABL-dependent expression of MCL-1 in Ba/F3 cells was counteracted by the mitogen-activated protein-kinase/extracellular signal-regulated kinase (MEK) inhibitor, PD98059, but not by the phosphoinositide 3-kinase inhibitor, LY294002. Identical results were obtained for constitutive expression of MCL-1 in primary CML cells and the CML-derived cell lines K562 and KU812. To investigate the role of MCL-1 as a survival-related target in CML cells, mcl-1 siRNA and mcl-1 antisense oligonucleotides (ASOs) were applied. The resulting down-regulation of MCL-1 was found to be assocd. with a substantial decrease in viability of K562 cells. Moreover, the mcl-1 ASO was found to synergize with imatinib in producing growth inhibition in these cells. Together, the authors' data identify MCL-1 as a BCR/ABL-dependent survival factor and interesting target in CML.

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16. 16

    Steven, L. G.; Klaus, P.; Jean-Luc, H.; Anderson, K. C. Mcl-1 regulation and its role in multiple myeloma. Cell Cycle 2004, 3, 1259– 1262,  DOI: 10.4161/cc.3.10.1196

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17. 17

    Song, L.; Coppola, D.; Livingston, S.; Cress, W. D.; Haura, E. B. Mcl-1 regulates survival and sensitivity to diverse apoptotic stimuli in human non-small cell lung cancer cells. Cancer Biol. Ther. 2005, 4, 267– 276,  DOI: 10.4161/cbt.4.3.1496

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    17

    Mcl-1 regulates survival and sensitivity to diverse apoptotic stimuli in human non-small cell lung cancer cells

    Song, Lanxi; Coppola, Domenico; Livingston, Sandy; Cress, Doug; Haura, Eric B.

    Cancer Biology & Therapy (2005), 4 (3), 267-276CODEN: CBTAAO; ISSN:1538-4047. (Landes Bioscience)

    Overexpression of anti-apoptotic Bcl-2 family members and deregulation of the pathways that regulate pro-apoptotic family members have been obsd. in non-small cell lung cancers (NSCLC). Previous reports have identified both Bcl-2 and Bcl-xL proteins as survival factors in lung cancer cells since redns. in these proteins can induce apoptosis and sensitize lung cancer cells to apoptosis induced by chemotherapy agents. Myeloid cell leukemia-1 (Mcl-1), another member of the Bcl-2 family, has been found to be a crit. survival factor in hematopoietic cells, yet little data exists for a role of Mcl-1 in human lung cancers. We used NSCLC cell lines to explore how Mcl-1 levels affect lung cancer cell survival and studied tumors from patients to det. expression patterns of Mcl-1. NSCLC cells express abundant Mcl-1 protein and depletion of Mcl-1 levels by antisense Mcl-1 oligonucleotides induces apoptosis in A549 and H1299 lung cancer cells. Redn. in Mcl-1 levels can sensitize lung cancer cells to apoptosis induced by cytotoxic agents as well as by ionizing radiation. Lung cancer cells overexpressing Mcl-1 are less sensitive to apoptosis induced by chemotherapeutic agents, ZD1839 (an inhibitor of EGFR tyrosine kinase) and Bcl-2 or Bcl-xL antisense oligonucleotides. We find that epidermal growth factor (EGF) can enhance Mcl-1 protein levels in an ERK-dependent manner. Signal transduction agents that reduce Mcl-1 levels correlated with their individual ability to induce apoptosis in lung cancer cells. Finally, NSCLC tumors taken directly from patients have elevated levels of Mcl-1 protein compared with normal adjacent lung tissue. Therefore, agents that target Mcl-1 can induce apoptosis and sensitize cells to apoptosis induced by cytotoxic agents. Mcl-1 protein is overexpressed in a subset of human NSCLC and enhanced levels of Mcl-1 may protect lung cancer cells from death induced by a variety of pro-apoptotic stimuli.

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18. 18

    Tong, J.; Wang, P.; Tan, S.; Chen, D.; Nikolovska-Coleska, Z.; Zou, F.; Yu, J.; Zhang, L. Mcl-1 degradation is required for targeted therapeutics to eradicate colon cancer cells. Cancer Res. 2017, 77, 2512– 2521,  DOI: 10.1158/0008-5472.CAN-16-3242

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    18

    Mcl-1 Degradation Is Required for Targeted Therapeutics to Eradicate Colon Cancer Cells

    Tong, Jingshan; Wang, Peng; Tan, Shuai; Chen, Dongshi; Nikolovska-Coleska, Zaneta; Zou, Fangdong; Yu, Jian; Zhang, Lin

    Cancer Research (2017), 77 (9), 2512-2521CODEN: CNREA8; ISSN:0008-5472. (American Association for Cancer Research)

    The Bcl-2 family protein Mcl-1 is often degraded in cancer cells subjected to effective therapeutic treatment, and defective Mcl-1 degrdn. has been assocd. with intrinsic and acquired drug resistance. However, a causal relationship between Mcl-1 degrdn. and anticancer drug responses has not been directly established, esp. in solid tumor cells where Mcl-1 inhibition alone is insufficient to trigger cell death. In this study, we present evidence that Mcl-1 participates directly in detg. effective therapeutic responses in colon cancer cells. In this setting, Mcl-1 degrdn. was induced by a variety of multikinase inhibitor drugs, where it relied upon GSK3β phosphorylation and FBW7-dependent ubiquitination. Specific blockade by genetic knock-in (KI) abolished apoptotic responses and conferred resistance to kinase inhibitors. Mcl-1-KI also suppressed the antiangiogenic and anti-hypoxic effects of kinase inhibitors in the tumor microenvironment. Interestingly, these same inhibitors also induced the BH3-only Bcl-2 family protein PUMA, which is required for apoptosis. Degrdn.-resistant Mcl-1 bound and sequestered PUMA from other prosurvival proteins to maintain cell survival, which was abolished by small-mol. Mcl-1 inhibitors. Our findings establish a pivotal role for Mcl-1 degrdn. in the response of colon cancer cells to targeted therapeutics, and they provide a useful rational platform to develop Mcl-1-targeting agents that can overcome drug resistance.

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19. 19

    Pepper, C.; Lin, T. T.; Pratt, G.; Hewamana, S.; Brennan, P.; Hiller, L.; Hills, R.; Ward, R.; Starczynski, J.; Austen, B.; Hooper, L.; Stankovic, T.; Fegan, C. Mcl-1 expression has in vitro and in vivo significance in chronic lymphocytic leukemia and is associated with other poor prognostic markers. Blood 2008, 112, 3807– 3817,  DOI: 10.1182/blood-2008-05-157131

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    19

    Mcl-1 expression has in vitro and in vivo significance in chronic lymphocytic leukemia and is associated with other poor prognostic markers

    Pepper, Chris; Lin, Thet Thet; Pratt, Guy; Hewamana, Saman; Brennan, Paul; Hiller, Louise; Hills, Robert; Ward, Rachel; Starczynski, Jane; Austen, Belinda; Hooper, Laura; Stankovic, Tatjana; Fegan, Chris

    Blood (2008), 112 (9), 3807-3817CODEN: BLOOAW; ISSN:0006-4971. (American Society of Hematology)

    Bcl-2 family proteins play a crit. role in the regulation of apoptosis in chronic lymphocytic leukemia (CLL). However, their assocn. with established prognostic markers is unknown. In this study, we analyzed the expression of Bcl-2, Bax, and Mcl-1 in 185 CLL patients and evaluated their relationship with other prognostic markers, in vitro sensitivity to fludarabine, and clin. outcome. Mcl-1 expression was significantly correlated with stage of disease (P < .001), lymphocyte doubling time (P = .01), VH gene mutation status (P < .001), CD38 expression (P < .001), and ZAP-70 expression (P = .003). In addn., Mcl-1 and Mcl-1/Bax ratios showed strong correlations with in vitro resistance to fludarabine (P = .005 and P < .001, resp.). Furthermore, elevated Mcl-1 expression and Mcl-1/Bax ratios were predictive of time to first treatment in the whole cohort (P < .001 and P < .001, resp.) and in stage A patients only (P = .002 and P = .001, resp.). Taken together, our data show that Mcl-1 is a key controller of in vitro drug resistance and is an important regulator of disease progression and outcome in CLL. It therefore represents a promising therapeutic target in this incurable condition. The close correlation between Mcl-1 expression and VH gene mutation status, CD38 expression, and ZAP-70 expression offers a biol. explanation for their assocn. with adverse prognosis.

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20. 20

    Zhou, P.; Qian, L.; Bieszczad, C. K.; Noelle, R.; Binder, M.; Levy, N. B.; Craig, R. W. Mcl-1 in transgenic mice promotes survival in a spectrum of hematopoietic cell types and immortalization in the myeloid lineage. Blood 1998, 92, 3226– 3239,  DOI: 10.1182/blood.V92.9.3226

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    20

    Mcl-1 in transgenic mice promotes survival in a spectrum of hematopoietic cell types and immortalization in the myeloid lineage

    Zhou, Ping; Qian, Liping; Bieszczad, Christine K.; Noelle, Randolph; Binder, Michael; Levy, Norman B.; Craig, Ruth W.

    Blood (1998), 92 (9), 3226-3239CODEN: BLOOAW; ISSN:0006-4971. (W. B. Saunders Co.)

    Mcl-1 is a member of the Bcl-2 family that is expressed in early monocyte differentiation and that can promote viability on transfection into immature myeloid cells. However, the effects of Mcl-1 are generally short lived compared with those of Bcl-2 and are not obvious in some transfectants. To further explore the effects of this gene, mice were produced that expressed Mcl-1 as a transgene in hematolymphoid tissues. The Mcl-1 transgene was found to cause moderate viability enhancement in a wide range of hematopoietic cell types, including lymphoid (B and T) as well as myeloid cells at both immature and mature stages of differentiation. However, enhanced hematopoietic capacity in transgenic bone marrow and spleen was not reflected in any change in pool sizes in the peripheral blood. In addn., among transgenic cells, mature T cells remained long lived compared with B cells and macrophages could live longer than either of these. Interestingly, when hematopoietic cells were maintained in tissue culture in the presence of interleukin-3, Mcl-1 enhanced the probability of outgrowth of continuously proliferating myeloid cell lines. Thus, Mcl-1 transgenic cells remained subject to normal in vivo homeostatic mechanisms controlling viable cell no., but these constraints could be overridden under specific conditions in vitro. Within the organism, Bcl-2 family members may act at "viability gates" along the differentiation continuum, functioning as part of a system for controlled hematopoietic cell amplification. Enforced expression of even a moderate viability-promoting member of this family such as Mcl-1, within a conducive intra- and extracellular environment in isolation from normal homeostatic constraints, can substantially increase the probability of cell immortalization.

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    Touzeau, C.; Maciag, P.; Amiot, M.; Moreau, P. Targeting Bcl-2 for the treatment of multiple myeloma. Leukemia 2018, 32, 1899– 1907,  DOI: 10.1038/s41375-018-0223-9

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    21

    Targeting Bcl-2 for the treatment of multiple myeloma

    Touzeau, Cyrille; Maciag, Paulo; Amiot, Martine; Moreau, Philippe

    Leukemia (2018), 32 (9), 1899-1907CODEN: LEUKED; ISSN:0887-6924. (Nature Research)

    Despite advances in the treatment of multiple myeloma, the disease still remains incurable for the majority of patients. The overexpression of anti-apoptotic proteins (i.e., Bcl-2, Bcl-XL or Mcl-1) is a hallmark of cancer and favors tumor cell survival and resistance to therapy. The oral drug venetoclax is the first-in-class Bcl-2-specific BH3 mimetic. In myeloma, in vitro sensitivity to venetoclax is mainly obsd. in plasma cells harboring the t(11;14) translocation, a mol. subgroup assocd. with high Bcl-2 and low Mcl-1/Bcl-XL expression. In addn. with Bcl-2 members expression profile, functional tests as BH3 profiling or in vitro BH3 mimetic drug testing also predict sensitivity to the drug. Phase 1 clin. trials recently confirmed the efficacy of venetoclax monotherapy in heavily pretreated myeloma patients, mostly in patients with t(11;14). In combination with the proteasome inhibitor bortezomib, venetoclax therapy was found to be feasible and allowed promising response rate in relapsed myeloma patients, independent of t(11;14) status. The present review summarizes the current knowledge, "from bench to bedside", about venetoclax for the treatment of multiple myeloma.

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22. 22

    Souers, A. J.; Leverson, J. D.; Boghaert, E. R.; Ackler, S. L.; Catron, N. D.; Chen, J.; Dayton, B. D.; Ding, H.; Enschede, S. H.; Fairbrother, W. J.; Huang, D. C. S.; Hymowitz, S. G.; Jin, S.; Khaw, S. L.; Kovar, P. J.; Lam, L. T.; Lee, J.; Maecker, H. L.; Marsh, K. C.; Mason, K. D.; Mitten, M. J.; Nimmer, P. M.; Oleksijew, A.; Park, C.-H.; Park, C. M.; Phillips, D. C.; Roberts, A. W.; Sampath, D.; Seymour, J. F.; Smith, M. L.; Sullivan, G. M.; Tahir, S. K.; Tse, C.; Wendt, M. D.; Xiao, Y.; Xue, J. C.; Zhang, H.; Humerickhouse, R. A.; Rosenberg, S. H.; Elmore, S. W. ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets. Nat. Med. 2013, 19, 202– 208,  DOI: 10.1038/nm.3048

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    22

    ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets

    Souers, Andrew J.; Leverson, Joel D.; Boghaert, Erwin R.; Ackler, Scott L.; Catron, Nathaniel D.; Chen, Jun; Dayton, Brian D.; Ding, Hong; Enschede, Sari H.; Fairbrother, Wayne J.; Huang, David C. S.; Hymowitz, Sarah G.; Jin, Sha; Khaw, Seong Lin; Kovar, Peter J.; Lam, Lloyd T.; Lee, Jackie; Maecker, Heather L.; Marsh, Kennan C.; Mason, Kylie D.; Mitten, Michael J.; Nimmer, Paul M.; Oleksijew, Anatol; Park, Chang H.; Park, Cheol-Min; Phillips, Darren C.; Roberts, Andrew W.; Sampath, Deepak; Seymour, John F.; Smith, Morey L.; Sullivan, Gerard M.; Tahir, Stephen K.; Tse, Chris; Wendt, Michael D.; Xiao, Yu; Xue, John C.; Zhang, Haichao; Humerickhouse, Rod A.; Rosenberg, Saul H.; Elmore, Steven W.

    Nature Medicine (New York, NY, United States) (2013), 19 (2), 202-208CODEN: NAMEFI; ISSN:1078-8956. (Nature Publishing Group)

    Proteins in the B cell CLL/lymphoma 2 (BCL-2) family are key regulators of the apoptotic process. This family comprises proapoptotic and prosurvival proteins, and shifting the balance toward the latter is an established mechanism whereby cancer cells evade apoptosis. The therapeutic potential of directly inhibiting prosurvival proteins was unveiled with the development of navitoclax, a selective inhibitor of both BCL-2 and BCL-2-like 1 (BCL-XL), which has shown clin. efficacy in some BCL-2-dependent hematol. cancers. However, concomitant on-target thrombocytopenia caused by BCL-XL inhibition limits the efficacy achievable with this agent. Here we report the re-engineering of navitoclax to create a highly potent, orally bioavailable and BCL-2-selective inhibitor, ABT-199. This compd. inhibits the growth of BCL-2-dependent tumors in vivo and spares human platelets. A single dose of ABT-199 in three patients with refractory chronic lymphocytic leukemia resulted in tumor lysis within 24 h. These data indicate that selective pharmacol. inhibition of BCL-2 shows promise for the treatment of BCL-2-dependent hematol. cancers.

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23. 23

    Quinn, B. A.; Dash, R.; Azab, B.; Sarkar, S.; Das, S. K.; Kumar, S.; Oyesanya, R. A.; Dasgupta, S.; Dent, P.; Grant, S.; Rahmani, M.; Curiel, D. T.; Dmitriev, I.; Hedvat, M.; Wei, J.; Wu, B.; Stebbins, J. L.; Reed, J. C.; Pellecchia, M.; Sarkar, D.; Fisher, P. B. Targeting Mcl-1 for the therapy of cancer. Expert Opin. Invest. Drugs 2011, 20, 1397– 1411,  DOI: 10.1517/13543784.2011.609167

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    23

    Targeting Mcl-1 for the therapy of cancer

    Quinn, Bridget A.; Dash, Rupesh; Azab, Belal; Sarkar, Siddik; Das, Swadesh K.; Kumar, Sachin; Oyesanya, Regina A.; Dasgupta, Santanu; Dent, Paul; Grant, Steven; Rahmani, Mohamed; Curiel, David T.; Dmitriev, Igor; Hedvat, Michael; Wei, Jun; Wu, Bainan; Stebbins, John L.; Reed, John C.; Pellecchia, Maurizio; Sarkar, Devanand; Fisher, Paul B.

    Expert Opinion on Investigational Drugs (2011), 20 (10), 1397-1411CODEN: EOIDER; ISSN:1354-3784. (Informa Healthcare)

    A review. Introduction:Human cancers are genetically and epigenetically heterogeneous and have the capacity to commandeer a variety of cellular processes to aid in their survival, growth and resistance to therapy. One strategy is to overexpress proteins that suppress apoptosis, such as the Bcl-2 family protein Mcl-1. The Mcl-1 protein plays a pivotal role in protecting cells from apoptosis and is overexpressed in a variety of human cancers.Areas covered:Targeting Mcl-1 for extinction in these cancers, using genetic and pharmacol. approaches, represents a potentially effectual means of developing new efficacious cancer therapeutics. Here we review the multiple strategies that have been employed in targeting this fundamental protein, as well as the significant potential these targeting agents provide in not only suppressing cancer growth, but also in reversing resistance to conventional cancer treatments.Expert opinion:We discuss the potential issues that arise in targeting Mcl-1 and other Bcl-2 anti-apoptotic proteins, as well problems with acquired resistance. The application of combinatorial approaches that involve inhibiting Mcl-1 and manipulation of addnl. signaling pathways to enhance therapeutic outcomes is also highlighted. The ability to specifically inhibit key genetic/epigenetic elements and biochem. pathways that maintain the tumor state represent a viable approach for developing rationally based, effective cancer therapies.

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    Akgul, C. Mcl-1 is a potential therapeutic target in multiple types of cancer. Cell. Mol. Life Sci. 2009, 66, 1326– 1336,  DOI: 10.1007/s00018-008-8637-6

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    24

    Mcl-1 is a potential therapeutic target in multiple types of cancer

    Akgul, C.

    Cellular and Molecular Life Sciences (2009), 66 (8), 1326-1336CODEN: CMLSFI; ISSN:1420-682X. (Birkhaeuser Verlag)

    A review. Resistance to apoptosis is a common challenge in human malignancies contributing to both progress of cancer and resistance to conventional therapeutics. Abnormalities in a variety of cell intrinsic and extrinsic mol. mechanisms cooperatively promote tumor formation. Therapeutic approaches that specifically target components of these mol. mechanisms are getting widespread attention. Mcl-1 is a highly expressed pro-survival protein in human malignancies and its cellular expression is tightly regulated via multiple mechanisms. Mcl-1 differs from other members of the Bcl-2 family in having a very short half-life. So inhibition of its expression and/or neutralization of its anti-apoptotic function will rapidly make Mcl-1-dependent cells more susceptible to apoptosis and provide an opportunity to combat several types of cancers. This review summarizes the current knowledge on the regulation of Mcl-1 expression and discusses the alternative approaches targeting Mcl-1 in human cancer cells whose survivals mainly depend on Mcl-1.

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25. 25

    Lessene, G.; Czabotar, P. E.; Colman, P. M. BCL-2 family antagonists for cancer therapy. Nat. Rev. Drug. Discov. 2008, 7, 989– 1000,  DOI: 10.1038/nrd2658

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    25

    BCL-2 family antagonists for cancer therapy

    Lessene, Guillaume; Czabotar, Peter E.; Colman, Peter M.

    Nature Reviews Drug Discovery (2008), 7 (12), 989-1000CODEN: NRDDAG; ISSN:1474-1776. (Nature Publishing Group)

    A review. Overexpression of members of the BCL-2 family of pro-survival proteins is commonly assocd. with unfavorable pathogenesis in cancer. The convergence of cytotoxic stress signals on the extended BCL-2 protein family provides the biol. rationale for directly targeting this family to induce apoptotic cell death. Recently, several compds. have been described that inhibit the interaction between BCL-2 family members and their natural ligand, a helical peptide sequence known as the BH3 domain. Here, we review preclin. and clin. data on these compds., and recommend four criteria that define antagonists of the BCL-2 protein family.

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26. 26

    Fire, E.; Gullá, S. V.; Grant, R. A.; Keating, A. E. Mcl-1-Bim complexes accommodate surprising point mutations via minor structural changes. Protein Sci. 2010, 19, 507– 519,  DOI: 10.1002/pro.329

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    26

    Mcl-1-Bim complexes accommodate surprising point mutations via minor structural changes

    Fire, Emiko; Gulla, Stefano V.; Grant, Robert A.; Keating, Amy E.

    Protein Science (2010), 19 (3), 507-519CODEN: PRCIEI; ISSN:1469-896X. (Wiley-Blackwell)

    Mcl-1 is an antiapoptotic Bcl-2-family protein that protects cells against death. Structures of Mcl-1, and of other anti-apoptotic Bcl-2 proteins, reveal a surface groove into which the α-helical BH3 regions of certain proapoptotic proteins can bind. Despite high overall structural conservation, differences in this groove afford binding specificity that is important for the mechanism of Bcl-2 family function. We report the crystal structure of human Mcl-1 bound to a BH3 peptide derived from human Bim and the structures for three complexes that accommodate large physicochem. changes at conserved Bim sites. The mutations had surprisingly modest effects on complex stability, and the structures show that Mcl-1 can undergo small changes to accommodate the mutant ligands. For example, a shift in a leucine side chain fills a hole left by an isoleucine-to-alanine mutation at the first hydrophobic buried position of Bim BH3. Larger changes are also obsd., with shifting of helix α3 accommodating an isoleucine-to-tyrosine mutation at this same position. We surveyed the variation in available Mcl-1 and Bcl-xL structures and obsd. moderate flexibility that is likely crit. for facilitating interactions of diverse BH3-only proteins with Mcl-1. With the antiapoptotic Bcl-2 family members attracting significant attention as therapeutic targets, these structures contribute to our growing understanding of how specificity is achieved and can help to guide the design of novel inhibitors that target Mcl-1.

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27. 27

    Gomez-Bougie, P.; Maiga, S.; Tessoulin, B.; Bourcier, J.; Bonnet, A.; Rodriguez, M. S.; Le Gouill, S.; Touzeau, C.; Moreau, P.; Pellat-Deceunynck, C.; Amiot, M. BH3-mimetic toolkit guides the respective use of BCL2 and MCL1 BH3-mimetics in myeloma treatment. Blood 2018, 132, 2656– 2669,  DOI: 10.1182/blood-2018-03-836718

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    27

    BH3-mimetic toolkit guides the respective use of BCL2 and MCL1 BH3-mimetics in myeloma treatment

    Gomez-Bougie, Patricia; Maiga, Sophie; Tessoulin, Benoit; Bourcier, Jessie; Bonnet, Antoine; Rodriguez, Manuel S.; Le Gouill, Steven; Touzeau, Cyrille; Moreau, Philippe; Pellat-Deceunynck, Catherine; Amiot, Martine

    Blood (2018), 132 (25), 2656-2669CODEN: BLOOAW; ISSN:1528-0020. (American Society of Hematology)

    BH3 mimetics are promising drugs for hematol. malignancies that trigger cell death by promoting the release of proapoptotic BCL2 family members from antiapoptotic proteins. Multiple myeloma is considered to be a disease dependent mainly on MCL1 for survival, based mostly on studies using cell lines. We used a BH3-mimetic toolkit to study the dependency on BCL2, BCLXL, or MCL1 in malignant plasma cells from 60 patients. Dependencies were analyzed using an unbiased BH3 mimetics cell-death clustering by k-means. In the whole cohort of patients, BCL2 dependency was mostly found in the CCND1 subgroup (83%). Of note, MCL1 dependence significantly increased from 33% at diagnosis to 69% at relapse, suggesting a plasticity of the cellular dependency favoring MCL1 dependencies at relapse. In addn., 35% of overall patient samples showed codependencies on either BCL2/MCL1 or BCLXL/MCL1. Finally, we identified a group of patients not targeted by any of the BH3 mimetics, predominantly at diagnosis in patients not presenting the common recurrent translocations. Interestingly, this complex was also dissocd. in A1210477-resistant cells, but free BAK was simultaneously recaptured by BCLXL, supporting the role of BCLXL in A1210477 resistance. In conclusion, our study opens the way to rationally use venetoclax and/or MCL1 BH3 mimetics for clin. evaluation in myeloma at both diagnosis and relapse.

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28. 28

    Zhang, Z.; Song, T.; Li, X.; Wu, Z.; Feng, Y.; Xie, F.; Liu, C.; Qin, J.; Chen, H. Novel soluble myeloid cell leukemia sequence 1 (Mcl-1) inhibitor (E,E)-2-(benzylaminocarbonyl)-3-styrylacrylonitrile (4g) developed using a fragment-based approach. Eur. J. Med. Chem. 2013, 59, 141– 149,  DOI: 10.1016/j.ejmech.2012.10.050

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    28

    Novel soluble myeloid cell leukemia sequence 1 (Mcl-1) inhibitor (E,E)-2-(benzylaminocarbonyl)-3-styrylacrylonitrile (4g) developed using a fragment-based approach

    Zhang, Zhichao; Song, Ting; Li, Xiangqian; Wu, Zhiyong; Feng, Yingang; Xie, Feibo; Liu, Chengwu; Qin, Jianquan; Chen, Hongbo

    European Journal of Medicinal Chemistry (2013), 59 (), 141-149CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    Based on a known nanomolar Bcl-2 homol. domain 3 (BH3) mimetic 3-thiomorpholin-8-oxo-8H-acenaphtho[1,2-b] pyrrole-9-carbonitrile (I, MW: 331), we applied a fragment-based approach to obtain BH3 mimetics with improved affinity and improved soly. in a water-ethanol (9:1) cosolvent. After the deconstruction of I, we obtained fragment cyanoacetamide (II), which was detd. to be a ligand efficiency (LE) hot part. After a rational optimization through fragment evolution beginning with fragment II, a smaller Mcl-1 inhibitor (E,E)-2-(benzylaminocarbonyl)-3-styrylacrylonitrile (III, MW: 288) with a 6-fold increase in affinity compared to I was obtained, as predicted by our optimization curve and identified by Mcl-1 protein NMR (NMR).

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29. 29

    Zhang, Z.; Liu, C.; Li, X.; Song, T.; Wu, Z.; Liang, X.; Zhao, Y.; Shen, X.; Chen, H. Fragment-based design, synthesis, and biological evaluation of N-substituted-5-(4-isopropylthiophenol)-2-hydroxynicotinamide derivatives as novel Mcl-1 inhibitors. Eur. J. Med. Chem. 2013, 60, 410– 420,  DOI: 10.1016/j.ejmech.2012.12.016

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    29

    Fragment-based design, synthesis, and biological evaluation of N-substituted-5-(4-isopropylthiophenol)-2-hydroxynicotinamide derivatives as novel Mcl-1 inhibitors

    Zhang, Zhichao; Liu, Chengwu; Li, Xiangqian; Song, Ting; Wu, Zhiyong; Liang, Xiaomeng; Zhao, Yan; Shen, Xiaoyun; Chen, Hongbo

    European Journal of Medicinal Chemistry (2013), 60 (), 410-420CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    We have previously reported a nanomolar inhibitor of antiapoptotic Mcl-1 protein, 3-thiomorpholin-8-oxo-8H-acenaphtho[1,2-b]pyrrole-9-carbonitrile (S1). S1 plays its function by binding to the BH3 groove of Mcl-1. Basing on this spacial structural characteristic, we developed a novel class of Mcl-1 inhibitor using fragment-based drug discovery approach. By dissecting S1, we identified 2-hydroxynicotinonitrile (4) with a 2-hydroxypyridine core as the starting fragment. In the following mol. growth, we used the ligand efficiency evaluation and fit quality score to assess the fragments. A novel potent compd., N-benzyl-5-(4-isopropylthiophenol)-2-hydroxyl nicotinamide (12c), which binds Mcl-1 with an IC50 value of 54 nM was obtained. Compd. 12c demonstrated a better aq. soly. than S1.

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    Liu, L.; Liu, R.; Yang, X.; Hou, X.; Fang, H. Design, synthesis and biological evaluation of tyrosine derivatives as Mcl-1 inhibitors. Eur. J. Med. Chem. 2020, 191, 112142,  DOI: 10.1016/j.ejmech.2020.112142

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    30

    Design, synthesis and biological evaluation of tyrosine derivatives as Mcl-1 inhibitors

    Liu, Lulu; Liu, Renshuai; Yang, Xinying; Hou, Xuben; Fang, Hao

    European Journal of Medicinal Chemistry (2020), 191 (), 112142CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    The upregulation of the protein myeloid cell leukemia-1 (Mcl-1) is closely assocd. with various human cancers, which can result in the evasion of apoptosis and a low survival rate. Therefore, developing Mcl-1 inhibitors has become a promising paradigm for cancer therapy. Herein, we designed and synthesized a novel series of tyrosine derivs., among which compds. (I) (R1 = 3,5-di-Me-4-Cl-Ph, X = H, R2 = OBut, n = 2; R1 = 3,5-di-Me-4-Cl-Ph, X = H, R2 = Ph, n = 1; R1 = naphthyl, X = Br, R2 = 4-Me-benzyl, n = 1) exhibited very high binding affinity to Mcl-1 with Ki values of 0.18, 0.27 and 0.23μM, resp. Interestingly, compd. I (R1 = 3,5-di-Me-4-Cl-Ph, X = H, R2 = Ph, n = 1) showed not only potent activity against Mcl-1 but also considerable selectivity over Bcl-2 and Bcl-xL, which was rationalized by mol. docking and fragment-centric topog. mapping (FCTM). It is worth noting that compds. I (R1 = 3,5-di-Me-4-Cl-Ph, X = H, R2 = OBut, n = 2; R1 = 3,5-di-Me-4-Cl-Ph, X = H, R2 = Ph, n = 1; R1 = naphthyl, X = Br, R2 = 4-Me-benzyl, n = 1) displayed potent antiproliferative activity against several cancer cell lines and could induce apoptosis of KM3 and HepG2 cells in a dose-dependent manner.

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31. 31

    Arkin, M. R.; Wells, J. A. Small-molecule inhibitors of protein-protein interactions: progressing towards the dream. Nat. Rev. Drug. Discov. 2004, 3, 301– 317,  DOI: 10.1038/nrd1343

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    31

    Small-molecule inhibitors of protein-protein interactions: progressing towards the dream

    Arkin, Michelle R.; Wells, James A.

    Nature Reviews Drug Discovery (2004), 3 (4), 301-317CODEN: NRDDAG; ISSN:1474-1776. (Nature Publishing Group)

    A review. Protein-protein interactions have a key role in most biol. processes, and offer attractive opportunities for therapeutic intervention. Developing small mols. that modulate protein-protein interactions is difficult, owing to issues such as the lack of well-defined binding pockets. Nevertheless, there was important progress in this endeavor in recent years. Here, the authors use illustrative examples to discuss general strategies for addressing the challenges inherent in the discovery and characterization of small-mol. inhibitors of protein-protein interactions.

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32. 32

    Horne, W. S.; Boersma, M. D.; Windsor, M. A.; Gellman, S. H. Sequence-based design of alpha/beta-peptide foldamers that mimic BH3 domains. Angew. Chem., Int. Ed. Engl. 2008, 47, 2853– 2856,  DOI: 10.1002/anie.200705315

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    Sequence-based design of alpha/beta-peptide foldamers that mimic BH3 domains

    Horne W Seth; Boersma Melissa D; Windsor Matthew A; Gellman Samuel H

    Angewandte Chemie (International ed. in English) (2008), 47 (15), 2853-6 ISSN:.

    There is no expanded citation for this reference.

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33. 33

    de Araujo, A. D.; Lim, J.; Wu, K.-C.; Xiang, Y.; Good, A. C.; Skerlj, R.; Fairlie, D. P. Bicyclic helical peptides as dual inhibitors selective for Bcl2A1 and Mcl-1 proteins. J. Med. Chem. 2018, 61, 2962– 2972,  DOI: 10.1021/acs.jmedchem.8b00010

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34. 34

    Muppidi, A.; Doi, K.; Edwardraja, S.; Drake, E. J.; Gulick, A. M.; Wang, H. G.; Lin, Q. Rational design of proteolytically stable, cell-permeable peptide-based selective Mcl-1 inhibitors. J. Am. Chem. Soc. 2012, 134, 14734– 14737,  DOI: 10.1021/ja306864v

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    Rational Design of Proteolytically Stable, Cell-Permeable Peptide-Based Selective Mcl-1 Inhibitors

    Muppidi, Avinash; Doi, Kenichiro; Edwardraja, Selvakumar; Drake, Eric J.; Gulick, Andrew M.; Wang, Hong-Gang; Lin, Qing

    Journal of the American Chemical Society (2012), 134 (36), 14734-14737CODEN: JACSAT; ISSN:0002-7863. (American Chemical Society)

    Direct chem. modifications provide a simple and effective means to "translate" bioactive helical peptides into potential therapeutics targeting intracellular protein-protein interactions. We previously showed that distance-matching bisaryl cross-linkers can reinforce peptide helixes contg. two cysteines at the i and i+7 positions and confer cell permeability to the cross-linked peptides. Here we report the first crystal structure of a biphenyl-cross-linked Noxa peptide in complex with its target Mcl-1 at 2.0 Å resoln. Guided by this structure, we remodeled the surface of this cross-linked peptide through side-chain substitution and N-methylation and obtained a pair of cross-linked peptides with substantially increased helicity, cell permeability, proteolytic stability, and cell-killing activity in Mcl-1-overexpressing U937 cells.

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    Stewart, M. L.; Fire, E.; Keating, A. E.; Walensky, L. D. The MCL-1 BH3 helix is an exclusive MCL-1 inhibitor and apoptosis sensitizer. Nat. Chem. Biol. 2010, 6, 595– 601,  DOI: 10.1038/nchembio.391

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    35

    The MCL-1 BH3 helix is an exclusive MCL-1 inhibitor and apoptosis sensitizer

    Stewart, Michelle L.; Fire, Emiko; Keating, Amy E.; Walensky, Loren D.

    Nature Chemical Biology (2010), 6 (8), 595-601CODEN: NCBABT; ISSN:1552-4450. (Nature Publishing Group)

    The development of selective inhibitors for discrete anti-apoptotic BCL-2 family proteins implicated in pathol. cell survival remains a formidable but pressing challenge. Such precisely tailored compds. would serve as mol. probes and targeted therapies to study and treat human diseases driven by specific anti-apoptotic blockades. In particular, MCL-1 has emerged as a major resistance factor in human cancer. By screening a library of stabilized alpha-helix of BCL-2 domains (SAHBs), we detd. that the MCL-1 BH3 helix is itself a potent and exclusive MCL-1 inhibitor. X-ray crystallog. and mutagenesis studies defined key binding and specificity determinants, including the capacity to harness the hydrocarbon staple to optimize affinity while preserving selectivity. MCL-1 SAHB directly targets MCL-1, neutralizes its inhibitory interaction with pro-apoptotic BAK and sensitizes cancer cells to caspase-dependent apoptosis. By leveraging nature's soln. to ligand selectivity, we generated an MCL-1-specific agent that defines the structural and functional features of targeted MCL-1 inhibition.

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36. 36

    Doi, K.; Li, R.; Sung, S. S.; Wu, H.; Liu, Y.; Manieri, W.; Krishnegowda, G.; Awwad, A.; Dewey, A.; Liu, X.; Amin, S.; Cheng, C.; Qin, Y.; Schonbrunn, E.; Daughdrill, G.; Loughran, T. P., Jr.; Sebti, S.; Wang, H. G. Discovery of marinopyrrole A (maritoclax) as a selective Mcl-1 antagonist that overcomes ABT-737 resistance by binding to and targeting Mcl-1 for proteasomal degradation. J. Biol. Chem. 2012, 287, 10224– 10235,  DOI: 10.1074/jbc.M111.334532

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    36

    Discovery of Marinopyrrole A (Maritoclax) as a Selective Mcl-1 Antagonist that Overcomes ABT-737 Resistance by Binding to and Targeting Mcl-1 for Proteasomal Degradation

    Doi, Kenichiro; Li, Rongshi; Sung, Shen-Shu; Wu, Hongwei; Liu, Yan; Manieri, Wanda; Krishnegowda, Gowdahalli; Awwad, Andy; Dewey, Alden; Liu, Xin; Amin, Shantu; Cheng, Chunwei; Qin, Yong; Schonbrunn, Ernst; Daughdrill, Gary; Loughran, Thomas P., Jr.; Sebti, Said; Wang, Hong-Gang

    Journal of Biological Chemistry (2012), 287 (13), 10224-10235CODEN: JBCHA3; ISSN:0021-9258. (American Society for Biochemistry and Molecular Biology)

    The anti-apoptotic Bcl-2 family of proteins, including Bcl-2, Bcl-XL and Mcl-1, are well-validated drug targets for cancer treatment. Several small mols. have been designed to interfere with Bcl-2 and its fellow pro-survival family members. While ABT-737 and its orally active analog ABT-263 are the most potent and specific inhibitors to date that bind Bcl-2 and Bcl-XL with high affinity but have a much lower affinity for Mcl-1, they are not very effective as single agents in certain cancer types because of elevated levels of Mcl-1. Accordingly, compds. that specifically target Mcl-1 may overcome this resistance. In this study, we identified and characterized the natural product marinopyrrole A as a novel Mcl-1-specific inhibitor and named it maritoclax. We found that maritoclax binds to Mcl-1, but not Bcl-XL, and is able to disrupt the interaction between Bim and Mcl-1. Moreover, maritoclax induces Mcl-1 degrdn. via the proteasome system, which is assocd. with the pro-apoptotic activity of maritoclax. Importantly, maritoclax selectively kills Mcl-1-dependent, but not Bcl-2- or Bcl-XL-dependent, leukemia cells and markedly enhances the efficacy of ABT-737 against hematol. malignancies, including K562, Raji, and multidrug-resistant HL60/VCR, by ∼60- to 2000-fold at 1-2 μM. Taken together, these results suggest that maritoclax represents a new class of Mcl-1 inhibitors, which antagonizes Mcl-1 and overcomes ABT-737 resistance by targeting Mcl-1 for degrdn.

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37. 37

    Lanning, M. E.; Yu, W.; Yap, J. L.; Chauhan, J.; Chen, L.; Whiting, E.; Pidugu, L. S.; Atkinson, T.; Bailey, H.; Li, W.; Roth, B. M.; Hynicka, L.; Chesko, K.; Toth, E. A.; Shapiro, P.; MacKerell, A. D., Jr.; Wilder, P. T.; Fletcher, S. Structure-based design of N-substituted 1-hydroxy-4-sulfamoyl-2-naphthoates as selective inhibitors of the Mcl-1 oncoprotein. Eur. J. Med. Chem. 2016, 113, 273– 292,  DOI: 10.1016/j.ejmech.2016.02.006

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    37

    Structure-based design of N-substituted 1-hydroxy-4-sulfamoyl-2-naphthoates as selective inhibitors of the Mcl-1 oncoprotein

    Lanning, Maryanna E.; Yu, Wenbo; Yap, Jeremy L.; Chauhan, Jay; Chen, Lijia; Whiting, Ellis; Pidugu, Lakshmi S.; Atkinson, Tyler; Bailey, Hala; Li, Willy; Roth, Braden M.; Hynicka, Lauren; Chesko, Kirsty; Toth, Eric A.; Shapiro, Paul; MacKerell, Alexander D., Jr.; Wilder, Paul T.; Fletcher, Steven

    European Journal of Medicinal Chemistry (2016), 113 (), 273-292CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    Structure-based drug design was utilized to develop novel, 1-hydroxy-2-naphthoate-based small-mol. inhibitors of Mcl-1. Ligand design was driven by exploiting a salt bridge with R263 and interactions with the p2 pocket of the protein. Significantly, target mols. were accessed in just two synthetic steps, suggesting further optimization will require minimal synthetic effort. Mol. modeling using the Site-Identification by Ligand Competitive Satn. (SILCS) approach was used to qual. direct ligand design as well as develop quant. models for inhibitor binding affinity to Mcl-1 and the Bcl-2 relative Bcl-xL as well as for the specificity of binding to the two proteins. Results indicated hydrophobic interactions in the p2 pocket dominated affinity of the most favorable binding ligand (3bl: Ki = 31 nM). Compds. were up to 19-fold selective for Mcl-1 over Bcl-xL. Selectivity of the inhibitors was driven by interactions with the deeper p2 pocket in Mcl-1 vs. Bcl-xL. The SILCS-based SAR of the present compds. represents the foundation for the development of Mcl-1 specific inhibitors with the potential to treat a wide range of solid tumors and hematol. cancers, including acute myeloid leukemia.

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38. 38

    Rescourio, G.; Gonzalez, A. Z.; Jabri, S.; Belmontes, B.; Moody, G.; Whittington, D.; Huang, X.; Caenepeel, S.; Cardozo, M.; Cheng, A. C.; Chow, D.; Dou, H.; Jones, A.; Kelly, R. C.; Li, Y.; Lizarzaburu, M.; Lo, M. C.; Mallari, R.; Meleza, C.; Rew, Y.; Simonovich, S.; Sun, D.; Turcotte, S.; Yan, X.; Wong, S. G.; Yanez, E.; Zancanella, M.; Houze, J.; Medina, J. C.; Hughes, P. E.; Brown, S. P. Discovery and in vivo evaluation of macrocyclic Mcl-1 inhibitors featuring an α-hydroxy phenylacetic acid pharmacophore or bioisostere. J. Med. Chem. 2019, 62, 10258– 10271,  DOI: 10.1021/acs.jmedchem.9b01310

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    38

    Discovery and in Vivo Evaluation of Macrocyclic Mcl-1 Inhibitors Featuring an α-Hydroxy Phenylacetic Acid Pharmacophore or Bioisostere

    Rescourio, Gwenaella; Gonzalez, Ana Z.; Jabri, Salman; Belmontes, Brian; Moody, Gordon; Whittington, Doug; Huang, Xin; Caenepeel, Sean; Cardozo, Mario; Cheng, Alan C.; Chow, David; Dou, Hannah; Jones, Adrie; Kelly, Ron C.; Li, Yihong; Lizarzaburu, Mike; Lo, Mei-Chu; Mallari, Rommel; Meleza, Cesar; Rew, Yosup; Simonovich, Scott; Sun, Daqing; Turcotte, Simon; Yan, Xuelei; Wong, Simon G.; Yanez, Evelyn; Zancanella, Manuel; Houze, Jonathan; Medina, Julio C.; Hughes, Paul E.; Brown, Sean P.

    Journal of Medicinal Chemistry (2019), 62 (22), 10258-10271CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Overexpression of the antiapoptotic protein Mcl-1 provides a survival advantage to some cancer cells, making inhibition of this protein an attractive therapeutic target for the treatment of certain types of tumors. Herein, we report our efforts toward the identification of a novel series of macrocyclic Mcl-1 inhibitors featuring an α-hydroxy phenylacetic acid pharmacophore or bioisostere. This work led to the discovery of 1(I), a potent Mcl-1 inhibitor (IC50 = 19 nM in an OPM-2 cell viability assay) with good pharmacokinetic properties and excellent in vivo efficacy in an OPM-2 multiple myeloma xenograft model.

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39. 39

    Song, T.; Wang, Z.; Ji, F.; Feng, Y.; Fan, Y.; Chai, G.; Li, X.; Li, Z.; Zhang, Z. Deactivation of Mcl-1 by dual-function small-molecule inhibitors targeting the bcl-2 homology 3 domain and facilitating mcl-1 ubiquitination. Angew. Chem., Int. Ed. Engl. 2016, 55, 14250– 14256,  DOI: 10.1002/anie.201606543

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    39

    Deactivation of Mcl-1 by Dual-Function Small-Molecule Inhibitors Targeting the Bcl-2 Homology 3 Domain and Facilitating Mcl-1 Ubiquitination

    Song Ting; Wang Ziqian; Chai Gaobo; Li Zhiqiang; Zhang Zhichao; Ji Fangling; Fan Yudan; Feng Yingang; Li Xiangqian

    Angewandte Chemie (International ed. in English) (2016), 55 (46), 14250-14256 ISSN:.

    By means of limited proteolysis assay, three-dimensional NMR, X-ray crystallography and alanine mutations, a dynamic region at the Q221R222N223 motif in the Bcl-2 homology 3 (BH3) domain of Mcl-1 has been identified as a conformational switch which controls Mcl-1 ubiquitination. Noxa(BH3) binding biases the QRN motif toward a helical conformation, thus leading to an enhanced in vitro ubiquitination of Mcl-1. In contrast, Bim(BH3) binding biases the QRN motif toward a nonhelical conformation, thus leading to the inhibition of ubiquitination. A dual function Mcl-1 inhibitor, which locates at the BH3 domain of Mcl-1 and forms hydrogen bond with His224 to drive a helical QRN conformation, so that it not only interferes with the pro-apoptotic partners, but also facilitates Mcl-1 ubiquitination in living cells, is described. As a result, this inhibitor manifests a more effective apoptosis induction in Mcl-1-dependent cancer cells than other inhibitors exhibiting a similar binding affinity with it.

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    Wang, Z.; He, N.; Guo, Z.; Niu, C.; Song, T.; Guo, Y.; Cao, K.; Wang, A.; Zhu, J.; Zhang, X.; Zhang, Z. Proteolysis targeting chimeras for the selective degradation of Mcl-1/Bcl-2 derived from nonselective target binding ligands. J. Med. Chem. 2019, 62, 8152– 8163,  DOI: 10.1021/acs.jmedchem.9b00919

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    40

    Proteolysis Targeting Chimeras for the Selective Degradation of Mcl-1/Bcl-2 Derived from Nonselective Target Binding Ligands

    Wang, Ziqian; He, Nianzhe; Guo, Zongwei; Niu, Cuili; Song, Ting; Guo, Yafei; Cao, Keke; Wang, Anhui; Zhu, Junjie; Zhang, Xiaodong; Zhang, Zhichao

    Journal of Medicinal Chemistry (2019), 62 (17), 8152-8163CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Proteolysis Targeting Chimera (PROTAC) recruits an E3 ligase to a target protein to induce its ubiquitination and subsequent degrdn. We reported the success in the development of two PROTACs (C3(I) and C5(II)) that potently and selectively induce the degrdn. of Mcl-1 and Bcl-2 (DC50 = 0.7 and 3.0 μM), resp., by introducing the E3 ligase cereblon (CRBN)-binding ligand pomalidomide to Mcl-1/Bcl-2 dual inhibitors S1-6 and Nap-1 with μM-range affinity. I-induced Mcl-1 ubiquitination translated into much more lethality in Mcl-1-dependent H23 cells than the most potent Mcl-1 occupancy-based inhibitor A-1210477 with nM-range affinity. Moreover, structure-activity relationship (SAR) anal. and mol. dynamic (MD) simulations discovered the structural basis for turning nonselective or promiscuous Bcl-2 family ligands into selective PROTACs. I and II exhibited reversible depletion in living cells, which provides a new potent toolkit for gain-of-function studies to probe the dynamic roles of Bcl-2 and Mcl-1 in apoptosis networks.

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41. 41

    Wang, Z.; Guo, Z.; Song, T.; Zhang, X.; He, N.; Liu, P.; Wang, P.; Zhang, Z. Proteome-wide identification of on- and off-targets of Bcl-2 inhibitors in native biological systems by using affinity-based probes (afbps). ChemBioChem 2018, 19, 2312– 2320,  DOI: 10.1002/cbic.201800380

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    41

    Proteome-Wide Identification of On- and Off-Targets of Bcl-2 Inhibitors in Native Biological Systems by Using Affinity-Based Probes (AfBPs)

    Wang, Ziqian; Guo, Zongwei; Song, Ting; Zhang, Xiaodong; He, Nianzhe; Liu, Peng; Wang, Peiran; Zhang, Zhichao

    ChemBioChem (2018), 19 (21), 2312-2320CODEN: CBCHFX; ISSN:1439-4227. (Wiley-VCH Verlag GmbH & Co. KGaA)

    Selective inhibition of proteins of the Bcl-2 family by small-mol. inhibitors is a promising new approach in drug discovery. However, information about how these mols. interact with their cellular targets (on- and off-) is highly limited. We have designed and synthesized photoreactive and "clickable" affinity-based probes (AfBPs)-Nap-2 and Nap-5-by introducing photo-crosslinkers onto Nap-1, a fluorescent deriv. of small-mol. Bcl-2 inhibitor S1-6. The resulting trifunctional probes Nap-2 and Nap-5 can enrich, visualize, and enable the identification of cellular on- and off-targets of Bcl-2 inhibitors both in vitro and in situ. Tubulin was validated as an off-target of Bcl-2 inhibitors (Nap-1 and S1-6) by large-scale cell-based proteome profiling and pull-down/western blotting (PD/WB) with Nap-2 and Nap-5. It was preliminarily illustrated to be a BH3-contg. protein because some well-known Bcl-2 inhibitors can block the labeling of tubulin by Nap-2.

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42. 42

    Zhang, Z.; Wu, G.; Xie, F.; Song, T.; Chang, X. 3-Thiomorpholin-8-oxo-8H-acenaphtho[1,2-b]pyrrole-9-carbonitrile (S1) based molecules as potent, dual inhibitors of B-cell lymphoma 2 (Bcl-2) and myeloid cell leukemia sequence 1 (Mcl-1): structure-based design and structure-activity relationship studies. J. Med. Chem. 2011, 54, 1101– 1105,  DOI: 10.1021/jm101181u

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    42

    3-Thiomorpholin-8-oxo-8H-acenaphtho[1,2-b]pyrrole-9-carbonitrile (S1) Based Molecules as Potent, Dual Inhibitors of B-Cell Lymphoma 2 (Bcl-2) and Myeloid Cell Leukemia Sequence 1 (Mcl-1): Structure-Based Design and Structure-Activity Relationship Studies

    Zhang, Zhichao; Wu, Guiye; Xie, Feibo; Song, Ting; Chang, Xilong

    Journal of Medicinal Chemistry (2011), 54 (4), 1101-1105CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    the authors recently described the discovery of a dual inhibitor of Bcl-2 and Mcl-1, 3-thiomorpholin-8-oxo-8H-acenaphtho[1,2-b]pyrrole-9-carbonitrile (3, S1). Here the authors report a structure-guided design in combination with structure-activity relationship studies to exploit the difference in the p2 binding pocket of Bcl-2 and Mcl-1, from which a novel dual inhibitor 3-(4-aminophenylthio)-8-oxo-8H-acenaphtho[1,2-b]pyrrole-9-carbonitrile (6h) was obtained, which showed significant enhanced IC50 value against Mcl-1 (5 nM), greater Mcl-1/Bak disruption potential, and accordingly a 10-fold increased cytotoxicity over 3.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BC3MXmtVeiuw%253D%253D&md5=08ad63a3a7bfb4afd477f63572d2f16c
43. 43

    Bruncko, M.; Song, X.; Tao, Z.; Kunzer, A. R. 7-nonsubstituted Indole Mcl-1 Inhibitors. WO2008130970Al, 2008.

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    Elmore, S. W.; Souers, A. J.; Bruncko, M.; Song, X.; Wang, X.; Hasvold, L. A.; Wang, L.; Kunzer, A. R.; Park, C.; Wendt, M. D.; Tao, Z. 7-sonsubstituted Indole Mcl-1 Inhibitors. WO2008131000A2, 2008.

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45. 45

    Friberg, A.; Vigil, D.; Zhao, B.; Daniels, R. N.; Burke, J. P.; Garcia-Barrantes, P. M.; Camper, D.; Chauder, B. A.; Lee, T.; Olejniczak, E. T.; Fesik, S. W. Discovery of potent myeloid cell leukemia 1 (Mcl-1) inhibitors using fragment-based methods and structure-based design. J. Med. Chem. 2013, 56, 15– 30,  DOI: 10.1021/jm301448p

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    45

    Discovery of Potent Myeloid Cell Leukemia 1 (Mcl-1) Inhibitors Using Fragment-Based Methods and Structure-Based Design

    Friberg, Anders; Vigil, Dominico; Zhao, Bin; Daniels, R. Nathan; Burke, Jason P.; Garcia-Barrantes, Pedro M.; Camper, DeMarco; Chauder, Brian A.; Lee, Taekyu; Olejniczak, Edward T.; Fesik, Stephen W.

    Journal of Medicinal Chemistry (2013), 56 (1), 15-30CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (Mcl-1), a member of the Bcl-2 family of proteins, is overexpressed and amplified in various cancers and promotes the aberrant survival of tumor cells that otherwise would undergo apoptosis. Here we describe the discovery of potent and selective Mcl-1 inhibitors using fragment-based methods and structure-based design. NMR-based screening of a large fragment library identified two chem. distinct hit series that bind to different sites on Mcl-1. Members of the two fragment classes were merged together to produce lead compds. that bind to Mcl-1 with a dissocn. const. of <100 nM with selectivity for Mcl-1 over Bcl-xL and Bcl-2. Structures of merged compds. when complexed to Mcl-1 were obtained by x-ray crystallog. and provide detailed information about the mol. recognition of small-mol. ligands binding Mcl-1. The compds. represent starting points for the discovery of clin. useful Mcl-1 inhibitors for the treatment of a wide variety of cancers.

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46. 46

    Burke, J. P.; Bian, Z.; Shaw, S.; Zhao, B.; Goodwin, C. M.; Belmar, J.; Browning, C. F.; Vigil, D.; Friberg, A.; Camper, D. V.; Rossanese, O. W.; Lee, T.; Olejniczak, E. T.; Fesik, S. W. Discovery of tricyclic indoles that potently inhibit Mcl-1 using fragment-based methods and structure-based design. J. Med. Chem. 2015, 58, 3794– 3805,  DOI: 10.1021/jm501984f

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    46

    Discovery of Tricyclic Indoles That Potently Inhibit Mcl-1 Using Fragment-Based Methods and Structure-Based Design

    Burke, Jason P.; Bian, Zhiguo; Shaw, Subrata; Zhao, Bin; Goodwin, Craig M.; Belmar, Johannes; Browning, Carrie F.; Vigil, Dominico; Friberg, Anders; Camper, DeMarco V.; Rossanese, Olivia W.; Lee, Taekyu; Olejniczak, Edward T.; Fesik, Stephen W.

    Journal of Medicinal Chemistry (2015), 58 (9), 3794-3805CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia-1 (Mcl-1) is an antiapoptotic member of the Bcl-2 family of proteins that is overexpressed and amplified in many cancers. Overexpression of Mcl-1 allows cancer cells to evade apoptosis and contributes to the resistance of cancer cells to be effectively treated with various chemotherapies. From an NMR-based screen of a large fragment library, several distinct chem. scaffolds that bind to Mcl-1 were discovered. Here, the authors describe the discovery of potent tricyclic 2-indole carboxylic acid inhibitors that exhibit single digit nanomolar binding affinity to Mcl-1 and greater than 1700-fold selectivity over Bcl-xL and greater than 100-fold selectivity over Bcl-2. X-ray structures of these compds. when complexed to Mcl-1 provide detailed information on how these small-mols. bind to the target, which was used to guide compd. optimization.

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47. 47

    Pelz, N. F.; Bian, Z.; Zhao, B.; Shaw, S.; Tarr, J. C.; Belmar, J.; Gregg, C.; Camper, D. V.; Goodwin, C. M.; Arnold, A. L.; Sensintaffar, J. L.; Friberg, A.; Rossanese, O. W.; Lee, T.; Olejniczak, E. T.; Fesik, S. W. Discovery of 2-indole-acylsulfonamide myeloid cell leukemia 1 (Mcl-1) inhibitors using fragment-based methods. J. Med. Chem. 2016, 59, 2054– 2066,  DOI: 10.1021/acs.jmedchem.5b01660

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    47

    Discovery of 2-Indole-acylsulfonamide Myeloid Cell Leukemia 1 (Mcl-1) Inhibitors Using Fragment-Based Methods

    Pelz, Nicholas F.; Bian, Zhiguo; Zhao, Bin; Shaw, Subrata; Tarr, James C.; Belmar, Johannes; Gregg, Claire; Camper, DeMarco V.; Goodwin, Craig M.; Arnold, Allison L.; Sensintaffar, John L.; Friberg, Anders; Rossanese, Olivia W.; Lee, Taekyu; Olejniczak, Edward T.; Fesik, Stephen W.

    Journal of Medicinal Chemistry (2016), 59 (5), 2054-2066CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia-1 (Mcl-1) is a member of the Bcl-2 family of proteins responsible for the regulation of programmed cell death. Amplification of Mcl-1 is a common genetic aberration in human cancer whose overexpression contributes to the evasion of apoptosis and is one of the major resistance mechanisms for many chemotherapies. Mcl-1 mediates its effects primarily through interactions with pro-apoptotic BH3 contg. proteins that achieve high affinity for the target by utilizing four hydrophobic pockets in its binding groove. Here we describe the discovery of Mcl-1 inhibitors using fragment-based methods and structure-based design. These novel inhibitors exhibit low nanomolar binding affinities to Mcl-1 and >500-fold selectivity over Bcl-xL. X-ray structures of lead Mcl-1 inhibitors when complexed to Mcl-1 provided detailed information on how these small-mols. bind to the target and were used extensively to guide compd. optimization.

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48. 48

    Shaw, S.; Bian, Z.; Zhao, B.; Tarr, J. C.; Veerasamy, N.; Jeon, K. O.; Belmar, J.; Arnold, A. L.; Fogarty, S. A.; Perry, E.; Sensintaffar, J. L.; Camper, D. V.; Rossanese, O. W.; Lee, T.; Olejniczak, E. T.; Fesik, S. W. Optimization of potent and selective tricyclic indole diazepinone myeloid cell leukemia-1 inhibitors using structure-based design. J. Med. Chem. 2018, 61, 2410– 2421,  DOI: 10.1021/acs.jmedchem.7b01155

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    48

    Optimization of Potent and Selective Tricyclic Indole Diazepinone Myeloid Cell Leukemia-1 Inhibitors Using Structure-Based Design

    Shaw, Subrata; Bian, Zhiguo; Zhao, Bin; Tarr, James C.; Veerasamy, Nagarathanam; Jeon, Kyu Ok; Belmar, Johannes; Arnold, Allison L.; Fogarty, Stuart A.; Perry, Evan; Sensintaffar, John L.; Camper, DeMarco V.; Rossanese, Olivia W.; Lee, Taekyu; Olejniczak, Edward T.; Fesik, Stephen W.

    Journal of Medicinal Chemistry (2018), 61 (6), 2410-2421CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (Mcl-1), an antiapoptotic member of the Bcl-2 family of proteins, has emerged as an attractive target for cancer therapy. Mcl-1 upregulation is often found in many human cancers and is assocd. with high tumor grade, poor survival, and resistance to chemotherapy. Here, we describe a series of potent and selective tricyclic indole diazepinone Mcl-1 inhibitors that were discovered and further optimized using structure-based design. These compds. exhibit picomolar binding affinity and mechanism-based cellular efficacy, including growth inhibition and caspase induction in Mcl-1-sensitive cells. Thus, they represent useful compds. to study the implication of Mcl-1 inhibition in cancer and serve as potentially useful starting points toward the discovery of anti-Mcl-1 therapeutics.

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49. 49

    Lee, T.; Christov, P. P.; Shaw, S.; Tarr, J. C.; Zhao, B.; Veerasamy, N.; Jeon, K. O.; Mills, J. J.; Bian, Z.; Sensintaffar, J. L.; Arnold, A. L.; Fogarty, S. A.; Perry, E.; Ramsey, H. E.; Cook, R. S.; Hollingshead, M.; Davis Millin, M.; Lee, K. M.; Koss, B.; Budhraja, A.; Opferman, J. T.; Kim, K.; Arteaga, C. L.; Moore, W. J.; Olejniczak, E. T.; Savona, M. R.; Fesik, S. W. Discovery of potent myeloid cell leukemia-1 (Mcl-1) inhibitors that demonstrate in vivo activity in mouse xenograft models of human cancer. J. Med. Chem. 2019, 62, 3971– 3988,  DOI: 10.1021/acs.jmedchem.8b01991

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    49

    Discovery of Potent Myeloid Cell Leukemia-1 (Mcl-1) Inhibitors That Demonstrate in Vivo Activity in Mouse Xenograft Models of Human Cancer

    Lee, Taekyu; Christov, Plamen P.; Shaw, Subrata; Tarr, James C.; Zhao, Bin; Veerasamy, Nagarathanam; Jeon, Kyu Ok; Mills, Jonathan J.; Bian, Zhiguo; Sensintaffar, John L.; Arnold, Allison L.; Fogarty, Stuart A.; Perry, Evan; Ramsey, Haley E.; Cook, Rebecca S.; Hollingshead, Melinda; Davis Millin, Myrtle; Lee, Kyung-min; Koss, Brian; Budhraja, Amit; Opferman, Joseph T.; Kim, Kwangho; Arteaga, Carlos L.; Moore, William J.; Olejniczak, Edward T.; Savona, Michael R.; Fesik, Stephen W.

    Journal of Medicinal Chemistry (2019), 62 (8), 3971-3988CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Overexpression of myeloid cell leukemia-1 (Mcl-1) in cancers correlates with high tumor grade and poor survival. Addnl., Mcl-1 drives intrinsic and acquired resistance to many cancer therapeutics, including B cell lymphoma 2 family inhibitors, proteasome inhibitors, and antitubulins. Therefore, Mcl-1 inhibition could serve as a strategy to target cancers that require Mcl-1 to evade apoptosis. Herein, we describe the use of structure-based design to discover a novel compd. (42) that robustly and specifically inhibits Mcl-1 in cell culture and animal xenograft models. Compd. 42 binds to Mcl-1 with picomolar affinity and inhibited growth of Mcl-1-dependent tumor cell lines in the nanomolar range. Compd. 42 also inhibited the growth of hematol. and triple neg. breast cancer xenografts at well-tolerated doses. These findings highlight the use of structure-based design to identify small mol. Mcl-1 inhibitors and support the use of 42 as a potential treatment strategy to block Mcl-1 activity and induce apoptosis in Mcl-1-dependent cancers.

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50. 50

    Ramsey, H. E.; Fischer, M. A.; Lee, T.; Gorska, A. E.; Arrate, M. P.; Fuller, L.; Boyd, K. L.; Strickland, S. A.; Sensintaffar, J.; Hogdal, L. J.; Ayers, G. D.; Olejniczak, E. T.; Fesik, S. W.; Savona, M. R. A novel Mcl-1 inhibitor combined with venetoclax rescues venetoclax-resistant acute myelogenous leukemia. Cancer. Discov. 2018, 8, 1566– 1581,  DOI: 10.1158/2159-8290.CD-18-0140

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    50

    A novel MCL1 inhibitor combined with venetoclax rescues venetoclax-resistant acute myelogenous leukemia

    Ramsey, Haley E.; Fischer, Melissa A.; Lee, Taekyu; Gorska, Agnieszka E.; Arrate, Maria Pia; Fuller, Londa; Boyd, Kelli L.; Strickland, Stephen A.; Sensintaffar, John; Hogdal, Leah J.; Ayers, Gregory D.; Olejniczak, Edward T.; Fesik, Stephen W.; Savona, Michael R.

    Cancer Discovery (2018), 8 (12), 1566-1581CODEN: CDAIB2; ISSN:2159-8274. (American Association for Cancer Research)

    Suppression of apoptosis by expression of antiapoptotic BCL2 family members is a hallmark of acute myeloblastic leukemia (AML). Induced myeloid leukemia cell differentiation protein (MCL1), an antiapoptotic BCL2 family member, is commonly upregulated in AML cells and is often a primary mode of resistance to treatment with the BCL2 inhibitor venetoclax. Here, we describe VU661013, a novel, potent, selective MCL1 inhibitor that destabilizes BIM/MCL1 assocn., leads to apoptosis in AML, and is active in venetoclax-resistant cells and patient-derived xenografts. In addn., VU661013 was safely combined with venetoclax for synergy in murine models of AML. Importantly, BH3 profiling of patient samples and drug-sensitivity testing ex vivo accurately predicted cellular responses to selective inhibitors of MCL1 or BCL2 and showed benefit of the combination. Taken together, these data suggest a strategy of rationally using BCL2 and MCL1 inhibitors in sequence or in combination in AML clin. trials.

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51. 51

    Bruncko, M.; Wang, L.; Sheppard, G. S.; Phillips, D. C.; Tahir, S. K.; Xue, J.; Erickson, S.; Fidanze, S.; Fry, E.; Hasvold, L.; Jenkins, G. J.; Jin, S.; Judge, R. A.; Kovar, P. J.; Madar, D.; Nimmer, P.; Park, C.; Petros, A. M.; Rosenberg, S. H.; Smith, M. L.; Song, X.; Sun, C.; Tao, Z. F.; Wang, X.; Xiao, Y.; Zhang, H.; Tse, C.; Leverson, J. D.; Elmore, S. W.; Souers, A. J. Structure-guided design of a series of MCL-1 inhibitors with high affinity and selectivity. J. Med. Chem. 2015, 58, 2180– 2194,  DOI: 10.1021/jm501258m

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    51

    Structure-Guided Design of a Series of MCL-1 Inhibitors with High Affinity and Selectivity

    Bruncko, Milan; Wang, Le; Sheppard, George S.; Phillips, Darren C.; Tahir, Stephen K.; Xue, John; Erickson, Scott; Fidanze, Steve; Fry, Elizabeth; Hasvold, Lisa; Jenkins, Gary J.; Jin, Sha; Judge, Russell A.; Kovar, Peter J.; Madar, David; Nimmer, Paul; Park, Chang; Petros, Andrew M.; Rosenberg, Saul H.; Smith, Morey L.; Song, Xiaohong; Sun, Chaohong; Tao, Zhi-Fu; Wang, Xilu; Xiao, Yu; Zhang, Haichao; Tse, Chris; Leverson, Joel D.; Elmore, Steven W.; Souers, Andrew J.

    Journal of Medicinal Chemistry (2015), 58 (5), 2180-2194CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (MCL-1) is a BCL-2 family protein that has been implicated in the progression and survival of multiple tumor types. Herein the authors report a series of MCL-1 inhibitors that emanated from a high throughput screening (HTS) hit and progressed via iterative cycles of structure-guided design. Advanced compds. from this series exhibited subnanomolar affinity for MCL-1 and excellent selectivity over other BCL-2 family proteins as well as multiple kinases and GPCRs. In a MCL-1 dependent human tumor cell line, administration of compd. I rapidly induced caspase activation with assocd. loss in cell viability. The small mols. described herein thus comprise effective tools for studying MCL-1 biol.

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52. 52

    Leverson, J. D.; Zhang, H.; Chen, J.; Tahir, S. K.; Phillips, D. C.; Xue, J.; Nimmer, P.; Jin, S.; Smith, M.; Xiao, Y.; Kovar, P.; Tanaka, A.; Bruncko, M.; Sheppard, G. S.; Wang, L.; Gierke, S.; Kategaya, L.; Anderson, D. J.; Wong, C.; Eastham-Anderson, J.; Ludlam, M. J. C.; Sampath, D.; Fairbrother, W. J.; Wertz, I.; Rosenberg, S. H.; Tse, C.; Elmore, S. W.; Souers, A. J. Potent and selective small-molecule MCL-1 inhibitors demonstrate on-target cancer cell killing activity as single agents and in combination with ABT-263 (navitoclax). Cell. Death. Dis. 2015, 6, e1590  DOI: 10.1038/cddis.2014.561

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    52

    Potent and selective small-molecule MCL-1 inhibitors demonstrate on-target cancer cell killing activity as single agents and in combination with ABT-263 (navitoclax)

    Leverson, J. D.; Zhang, H.; Chen, J.; Tahir, S. K.; Phillips, D. C.; Xue, J.; Nimmer, P.; Jin, S.; Smith, M.; Xiao, Y.; Kovar, P.; Tanaka, A.; Bruncko, M.; Sheppard, G. S.; Wang, L.; Gierke, S.; Kategaya, L.; Anderson, D. J.; Wong, C.; Eastham-Anderson, J.; Ludlam, M. J. C.; Sampath, D.; Fairbrother, W. J.; Wertz, I.; Rosenberg, S. H.; Tse, C.; Elmore, S. W.; Souers, A. J.

    Cell Death & Disease (2015), 6 (1), e1590CODEN: CDDEA4; ISSN:2041-4889. (Nature Publishing Group)

    The anti-apoptotic protein MCL-1 is a key regulator of cancer cell survival and a known resistance factor for small-mol. BCL-2 family inhibitors such as ABT-263 (navitoclax), making it an attractive therapeutic target. However, directly inhibiting this target requires the disruption of high-affinity protein-protein interactions, and therefore designing small mols. potent enough to inhibit MCL-1 in cells has proven extremely challenging. Here, we describe a series of indole-2-carboxylic acids, exemplified by the compd. A-1210477, that bind to MCL-1 selectively and with sufficient affinity to disrupt MCL-1-BIM complexes in living cells. A-1210477 induces the hallmarks of intrinsic apoptosis and demonstrates single agent killing of multiple myeloma and non-small cell lung cancer cell lines demonstrated to be MCL-1 dependent by BH3 profiling or siRNA rescue expts. As predicted, A-1210477 synergizes with the BCL-2/BCL-XL inhibitor navitoclax to kill a variety of cancer cell lines. This work represents the first description of small-mol. MCL-1 inhibitors with sufficient potency to induce clear on-target cellular activity. It also demonstrates the utility of these mols. as chem. tools for dissecting the basic biol. of MCL-1 and the promise of small-mol. MCL-1 inhibitors as potential therapeutics for the treatment of cancer.

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53. 53

    Xiao, Y.; Nimmer, P.; Sheppard, G. S.; Bruncko, M.; Hessler, P.; Lu, X.; Roberts-Rapp, L.; Pappano, W. N.; Elmore, S. W.; Souers, A. J.; Leverson, J. D.; Phillips, D. C. Mcl-1 is a key determinant of breast cancer cell survival: validation of Mcl-1 dependency utilizing a highly selective small molecule inhibitor. Mol. Cancer Ther. 2015, 14, 1837– 1847,  DOI: 10.1158/1535-7163.MCT-14-0928

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    53

    MCL-1 Is a Key Determinant of Breast Cancer Cell Survival: Validation of MCL-1 Dependency Utilizing a Highly Selective Small Molecule Inhibitor

    Xiao, Yu; Nimmer, Paul; Sheppard, George S.; Bruncko, Milan; Hessler, Paul; Lu, Xin; Roberts-Rapp, Lisa; Pappano, William N.; Elmore, Steven W.; Souers, Andrew J.; Leverson, Joel D.; Phillips, Darren C.

    Molecular Cancer Therapeutics (2015), 14 (8), 1837-1847CODEN: MCTOCF; ISSN:1535-7163. (American Association for Cancer Research)

    Hyperexpression of antiapoptotic BCL-2 family proteins allows cells to survive despite the receipt of signals that would ordinarily induce their deletion, a facet frequently exploited by tumors. Tumors addicted to the BCL-2 family proteins for survival are now being targeted therapeutically. For example, navitoclax, a BCL-2/BCL-XL/BCL-W inhibitor, is currently in phase I/II clin. trials in numerous malignancies. However, the related family member, MCL-1, limits the efficacy of navitoclax and other chemotherapeutic agents. In the present study, we identify breast cancer cell lines that depend upon MCL-1 for survival and subsequently det. the mechanism of apoptosis mediated by the MCL-1 selective inhibitor A-1210477. We demonstrate that apoptosis resulting from a loss in MCL-1 function requires expression of the proapoptotic protein BAK. However, expression of BCL-XL can limit apoptosis resulting from loss in MCL-1 function through sequestration of free BIM. Finally, we demonstrate substantial synergy between navitoclax and MCL-1 siRNA, the direct MCL-1 inhibitor A-1210477, or the indirect MCL-1 inhibitor flavopiridol, highlighting the therapeutic potential for inhibiting BCL-XL and MCL-1 in breast cancer. Mol Cancer Ther; 14(8); 1837-47. cpr2015 AACR.

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54. 54

    Akçay, G.; Belmonte, M. A.; Aquila, B.; Chuaqui, C.; Hird, A. W.; Lamb, M. L.; Rawlins, P. B.; Su, N.; Tentarelli, S.; Grimster, N. P.; Su, Q. Inhibition of Mcl-1 through covalent modification of a noncatalytic lysine side chain. Nat. Chem. Biol. 2016, 12, 931– 936,  DOI: 10.1038/nchembio.2174

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    Inhibition of Mcl-1 through covalent modification of a noncatalytic lysine side chain

    Akcay, Gizem; Belmonte, Matthew A.; Aquila, Brian; Chuaqui, Claudio; Hird, Alexander W.; Lamb, Michelle L.; Rawlins, Philip B.; Su, Nancy; Tentarelli, Sharon; Grimster, Neil P.; Su, Qibin

    Nature Chemical Biology (2016), 12 (11), 931-936CODEN: NCBABT; ISSN:1552-4450. (Nature Publishing Group)

    Targeted covalent inhibition of disease-assocd. proteins has become a powerful methodol. in the field of drug discovery, leading to the approval of new therapeutics. Nevertheless, current approaches are often limited owing to their reliance on a cysteine residue to generate the covalent linkage. Here the authors used aryl boronic acid carbonyl warheads to covalently target a noncatalytic lysine side chain, and generated to the knowledge the first reversible covalent inhibitors for Mcl-1, a protein-protein interaction (PPI) target that has proven difficult to inhibit via traditional medicinal chem. strategies. These covalent binders exhibited improved potency in comparison to noncovalent congeners, as demonstrated in biochem. and cell-based assays. The authors identified Lys234 as the residue involved in covalent modification, via point mutation. The covalent binders discovered in this study will serve as useful starting points for the development of Mcl-1 therapeutics and probes to interrogate Mcl-1-dependent biol. phenomena.

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55. 55

    Papatzimas, J. W.; Gorobets, E.; Maity, R.; Muniyat, M. I.; MacCallum, J. L.; Neri, P.; Bahlis, N. J.; Derksen, D. J. From inhibition to degradation: targeting the antiapoptotic protein myeloid cell leukemia 1 (Mcl-1). J. Med. Chem. 2019, 62, 5522– 5540,  DOI: 10.1021/acs.jmedchem.9b00455

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    From Inhibition to Degradation: Targeting the Antiapoptotic Protein Myeloid Cell Leukemia 1 (MCL1)

    Papatzimas, James W.; Gorobets, Evgueni; Maity, Ranjan; Muniyat, Mir Ishruna; MacCallum, Justin L.; Neri, Paola; Bahlis, Nizar J.; Derksen, Darren J.

    Journal of Medicinal Chemistry (2019), 62 (11), 5522-5540CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Protein-protein interactions (PPIs) have emerged as significant targets for therapeutic development, owing to their crit. nature in diverse biol. processes. An ideal PPI-based target is the protein myeloid cell leukemia 1 (MCL1), a crit. prosurvival factor in cancers such as multiple myeloma where MCL1 levels directly correlate to disease progression. Current strategies for halting the antiapoptotic properties of MCL1 revolve around inhibiting its sequestration of proapoptotic factors. Existing inhibitors disrupt endogenous regulatory proteins; however, this strategy actually increases MCL1 protein levels. Here, the authors show the development of hetero-bifunctional small mols. capable of selectively targeting MCL1 using a proteolysis targeting chimera (PROTAC) methodol. leading to successful degrdn. The authors confirmed the involvement of the E3 ligase CUL4A-DDB1 cereblon ubiquitination pathway, making these PROTACs a first step toward a new class of antiapoptotic B-cell lymphoma 2 family protein degraders.

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56. 56

    Johannes, J. W.; Bates, S.; Beigie, C.; Belmonte, M. A.; Breen, J.; Cao, S.; Centrella, P. A.; Clark, M. A.; Cuozzo, J. W.; Dumelin, C. E.; Ferguson, A. D.; Habeshian, S.; Hargreaves, D.; Joubran, C.; Kazmirski, S.; Keefe, A. D.; Lamb, M. L.; Lan, H.; Li, Y.; Ma, H.; Mlynarski, S.; Packer, M. J.; Rawlins, P. B.; Robbins, D. W.; Shen, H.; Sigel, E. A.; Soutter, H. H.; Su, N.; Troast, D. M.; Wang, H.; Wickson, K. F.; Wu, C.; Zhang, Y.; Zhao, Q.; Zheng, X.; Hird, A. W. Structure based design of non-natural peptidic macrocyclic Mcl-1 inhibitors. ACS Med. Chem. Lett. 2017, 8, 239– 244,  DOI: 10.1021/acsmedchemlett.6b00464

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    56

    Structure based design of non-natural peptidic macrocyclic Mcl-1 inhibitors

    Johannes, Jeffrey W.; Bates, Stephanie; Beigie, Carl; Belmonte, Matt; Breen, John; Cao, Shenggen; Centrella, Paolo A.; Clark, Matthew A.; Cuozzo, John W.; Dumelin, Christoph E.; Ferguson, Andrew D.; Habeshian, Sevan; Hargreaves, David; Joubran, Camil; Kazmirski, Steven; Keefe, Anthony D.; Lamb, Michelle L.; Lan, Haiye; Li, Yunxia; Ma, Hao; Mlynarski, Scott; Packer, Martin J.; Rawlins, Philip B.; Robbins, Daniel W.; Shen, Haidong; Sigel, Eric A.; Soutter, Holly H.; Su, Nancy; Troast, Dawn M.; Wang, Haiyun; Wickson, Kate F.; Wu, Chengyan; Zhang, Ying; Zhao, Qiuying; Zheng, Xiaolan; Hird, Alexander W.

    ACS Medicinal Chemistry Letters (2017), 8 (2), 239-244CODEN: AMCLCT; ISSN:1948-5875. (American Chemical Society)

    Mcl-1 is a pro-apoptotic BH3 protein family member similar to Bcl-2 and Bcl-xL. Overexpression of Mcl-1 is often seen in various tumors and allows cancer cells to evade apoptosis. Here we report the discovery and optimization of a series of non-natural peptide Mcl-1 inhibitors. Screening of DNA-encoded libraries resulted in hit compd. (I), a 1.5 μM Mcl-1 inhibitor. A subsequent crystal structure demonstrated that compd. I bound to Mcl-1 in a β-turn conformation, such that the two ends of the peptide were close together. This proximity allowed for the linking of the two ends of the peptide to form a macrocycle. Macrocyclization resulted in an approx. 10-fold improvement in binding potency. Further exploration of a key hydrophobic interaction with Mcl-1 protein and also with the moiety that engages Arg256 led to addnl. potency improvements. The use of protein-ligand crystal structures and binding kinetics contributed to the design and understanding of the potency gains. Optimized compd. (II) is a <3 nM Mcl-1 inhibitor, while inhibiting Bcl-2 at only 5 μM and Bcl-xL at >99 μM, and induces cleaved caspase-3 in MV4-11 cells with an IC50 of 3 μM after 6 h.

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    Tron, A. E.; Belmonte, M. A.; Adam, A.; Aquila, B. M.; Boise, L. H.; Chiarparin, E.; Cidado, J.; Embrey, K. J.; Gangl, E.; Gibbons, F. D.; Gregory, G. P.; Hargreaves, D.; Hendricks, J. A.; Johannes, J. W.; Johnstone, R. W.; Kazmirski, S. L.; Kettle, J. G.; Lamb, M. L.; Matulis, S. M.; Nooka, A. K.; Packer, M. J.; Peng, B.; Rawlins, P. B.; Robbins, D. W.; Schuller, A. G.; Su, N.; Yang, W.; Ye, Q.; Zheng, X.; Secrist, J. P.; Clark, E. A.; Wilson, D. M.; Fawell, S. E.; Hird, A. W. Discovery of Mcl-1-specific inhibitor AZD5991 and preclinical activity in multiple myeloma and acute myeloid leukemia. Nat. Commun. 2018, 9, 5341,  DOI: 10.1038/s41467-018-07551-w

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    Discovery of Mcl-1-specific inhibitor AZD5991 and preclinical activity in multiple myeloma and acute myeloid leukemia

    Tron, Adriana E.; Belmonte, Matthew A.; Adam, Ammar; Aquila, Brian M.; Boise, Lawrence H.; Chiarparin, Elisabetta; Cidado, Justin; Embrey, Kevin J.; Gangl, Eric; Gibbons, Francis D.; Gregory, Gareth P.; Hargreaves, David; Hendricks, J. Adam; Johannes, Jeffrey W.; Johnstone, Ricky W.; Kazmirski, Steven L.; Kettle, Jason G.; Lamb, Michelle L.; Matulis, Shannon M.; Nooka, Ajay K.; Packer, Martin J.; Peng, Bo; Rawlins, Philip B.; Robbins, Daniel W.; Schuller, Alwin G.; Su, Nancy; Yang, Wenzhan; Ye, Qing; Zheng, Xiaolan; Secrist, J. Paul; Clark, Edwin A.; Wilson, David M.; Fawell, Stephen E.; Hird, Alexander W.

    Nature Communications (2018), 9 (1), 5341CODEN: NCAOBW; ISSN:2041-1723. (Nature Research)

    Mcl-1 is a member of the Bcl-2 family of proteins that promotes cell survival by preventing induction of apoptosis in many cancers. High expression of Mcl-1 causes tumorigenesis and resistance to anticancer therapies highlighting the potential of Mcl-1 inhibitors as anticancer drugs. Here, we describe AZD5991, a rationally designed macrocyclic mol. with high selectivity and affinity for Mcl-1 currently in clin. development. Our studies demonstrate that AZD5991 binds directly to Mcl-1 and induces rapid apoptosis in cancer cells, most notably myeloma and acute myeloid leukemia, by activating the Bak-dependent mitochondrial apoptotic pathway. AZD5991 shows potent antitumor activity in vivo with complete tumor regression in several models of multiple myeloma and acute myeloid leukemia after a single tolerated dose as monotherapy or in combination with bortezomib or venetoclax. Based on these promising data, a Phase I clin. trial has been launched for evaluation of AZD5991 in patients with hematol. malignancies (NCT03218683).

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    Sale, M. J.; Minihane, E.; Monks, N. R.; Gilley, R.; Richards, F. M.; Schifferli, K. P.; Andersen, C. L.; Davies, E. J.; Vicente, M. A.; Ozono, E.; Markovets, A.; Dry, J. R.; Drew, L.; Flemington, V.; Proia, T.; Jodrell, D. I.; Smith, P. D.; Cook, S. J. Targeting melanoma’s MCL1 bias unleashes the apoptotic potential of BRAF and ERK1/2 pathway inhibitors. Nat. Commun. 2019, 10, 5167,  DOI: 10.1038/s41467-019-12409-w

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    Targeting melanoma's MCL1 bias unleashes the apoptotic potential of BRAF and ERK1/2 pathway inhibitors

    Sale Matthew J; Minihane Emma; Gilley Rebecca; Ozono Eiko; Cook Simon J; Monks Noel R; Schifferli Kevin P; Richards Frances M; Jodrell Duncan I; Andersen Courtney L; Markovets Aleksandra; Dry Jonathan R; Drew Lisa; Proia Theresa; Davies Emma J; Flemington Vikki; Smith Paul D; Vicente Mario Aladren

    Nature communications (2019), 10 (1), 5167 ISSN:.

    BRAF and MEK1/2 inhibitors are effective in melanoma but resistance inevitably develops. Despite increasing the abundance of pro-apoptotic BIM and BMF, ERK1/2 pathway inhibition is predominantly cytostatic, reflecting residual pro-survival BCL2 family activity. Here, we show that uniquely low BCL-XL expression in melanoma biases the pro-survival pool towards MCL1. Consequently, BRAF or MEK1/2 inhibitors are synthetic lethal with the MCL1 inhibitor AZD5991, driving profound tumour cell death that requires BAK/BAX, BIM and BMF, and inhibiting tumour growth in vivo. Combination of ERK1/2 pathway inhibitors with BCL2/BCL-w/BCL-XL inhibitors is stronger in CRC, correlating with a low MCL1:BCL-XL ratio; indeed the MCL1:BCL-XL ratio is predictive of ERK1/2 pathway inhibitor synergy with MCL1 or BCL2/BCL-w/BCL-XL inhibitors. Finally, AZD5991 delays acquired BRAFi/MEKi resistance and enhances the efficacy of an ERK1/2 inhibitor in a model of acquired BRAFi + MEKi resistance. Thus combining ERK1/2 pathway inhibitors with MCL1 antagonists in melanoma could improve therapeutic index and patient outcomes.

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59. 59

    Zhang, H.; Nakauchi, Y.; Köhnke, T.; Stafford, M.; Bottomly, D.; Thomas, R.; Wilmot, B.; McWeeney, S. K.; Majeti, R.; Tyner, J. W. Integrated analysis of patient samples identifies biomarkers for venetoclax efficacy and combination strategies in acute myeloid leukemia. Nat. Cancer. 2020, 1, 826– 839,  DOI: 10.1038/s43018-020-0103-x

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    59

    Integrated analysis of patient samples identifies biomarkers for venetoclax efficacy and combination strategies in acute myeloid leukemia

    Zhang Haijiao; Tyner Jeffrey W; Nakauchi Yusuke; Kohnke Thomas; Stafford Melissa; Thomas Rozario; Majeti Ravindra; Bottomly Daniel; Wilmot Beth; McWeeney Shannon K

    Nature cancer (2020), 1 (8), 826-839 ISSN:.

    Deregulation of the BCL2 gene family plays an important role in the pathogenesis of acute myeloid leukemia (AML). The BCL2 inhibitor, venetoclax, has received FDA approval for the treatment of AML. However, upfront and acquired drug resistance ensues due, in part, to the clinical and genetic heterogeneity of AML, highlighting the importance of identifying biomarkers to stratify patients onto the most effective therapies. By integrating clinical characteristics, exome and RNA sequencing, and inhibitor data from primary AML patient samples, we determined that myelomonocytic leukemia, upregulation of BCL2A1 and CLEC7A, as well as mutations of PTPN11 and KRAS conferred resistance to venetoclax and multiple venetoclax combinations. Venetoclax in combination with an MCL1 inhibitor AZD5991 induced synthetic lethality and circumvented venetoclax resistance.

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60. 60

    Caenepeel, S.; Brown, S. P.; Belmontes, B.; Moody, G.; Keegan, K. S.; Chui, D.; Whittington, D. A.; Huang, X.; Poppe, L.; Cheng, A. C.; Cardozo, M.; Houze, J.; Li, Y.; Lucas, B.; Paras, N. A.; Wang, X.; Taygerly, J. P.; Vimolratana, M.; Zancanella, M.; Zhu, L.; Cajulis, E.; Osgood, T.; Sun, J.; Damon, L.; Egan, R. K.; Greninger, P.; McClanaghan, J. D.; Gong, J.; Moujalled, D.; Pomilio, G.; Beltran, P.; Benes, C. H.; Roberts, A. W.; Huang, D. C.; Wei, A.; Canon, J.; Coxon, A.; Hughes, P. E. AMG 176, a selective Mcl-1 inhibitor, is effective in hematologic cancer models alone and in combination with established therapies. Cancer. Discov. 2018, 8, 1582– 1597,  DOI: 10.1158/2159-8290.CD-18-0387

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    AMG 176, a selective MCL1 inhibitor, is effective in hematologic cancer models alone and in combination with established therapies

    Caenepeel, Sean; Brown, Sean P.; Belmontes, Brian; Moody, Gordon; Keegan, Kathleen S.; Chui, Danny; Whittington, Douglas A.; Huang, Xin; Poppe, Leszek; Cheng, Alan C.; Cardozo, Mario; Houze, Jonathan; Li, Yunxiao; Lucas, Brian; Paras, Nick A.; Wang, Xianghong; Taygerly, Joshua P.; Vimolratana, Marc; Zancanella, Manuel; Zhu, Liusheng; Cajulis, Elaina; Osgood, Tao; Sun, Jan; Damon, Leah; Egan, Regina K.; Greninger, Patricia; McClanaghan, Joseph D.; Gong, Jianan; Moujalled, Donia; Pomilio, Giovanna; Beltran, Pedro; Benes, Cyril H.; Roberts, Andrew W.; Huang, David C.; Wei, Andrew; Canon, Jude; Coxon, Angela; Hughes, Paul E.

    Cancer Discovery (2018), 8 (12), 1582-1597CODEN: CDAIB2; ISSN:2159-8274. (American Association for Cancer Research)

    The prosurvival BCL2 family member MCL1 is frequently dysregulated in cancer. To overcome the significant challenges assocd. with inhibition of MCL1 protein-protein interactions, we rigorously applied small-mol. conformational restriction, which culminated in the discovery of AMG 176, the first selective MCL1 inhibitor to be studied in humans. We demonstrate that MCL1 inhibition induces a rapid and committed step toward apoptosis in subsets of hematol. cancer cell lines, tumor xenograft models, and primary patient samples. With the use of a human MCL1 knock-in mouse, we demonstrate that MCL1 inhibition at active doses of AMG 176 is tolerated and correlates with clear pharmacodynamic effects, demonstrated by redns. in B cells, monocytes, and neutrophils. Furthermore, the combination of AMG 176 and venetoclax is synergistic in acute myeloid leukemia (AML) tumor models and in primary patient samples at tolerated doses. These results highlight the therapeutic promise of AMG 176 and the potential for combinations with other BH3 mimetics.

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61. 61

    Lu, X.; Liu, Y. C.; Orvig, C.; Liang, H.; Chen, Z. F. Discovery of a Copper-Based Mcl-1 Inhibitor as an Effective Antitumor Agent. J. Med. Chem. 2020, 63, 9154– 9167,  DOI: 10.1021/acs.jmedchem.9b02047

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    61

    Discovery of a Copper-Based Mcl-1 Inhibitor as an Effective Antitumor Agent

    Lu, Xing; Liu, Yan-Cheng; Orvig, Chris; Liang, Hong; Chen, Zhen-Feng

    Journal of Medicinal Chemistry (2020), 63 (17), 9154-9167CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (Mcl-1), which belongs to the Bcl-2 family of prosurvival proteins, is a key regulator of cancer cell survival. To date, few drug-like Mcl-1 inhibitors have been reported. Herein, it is reported the prepn. of 10 copper complexes with 9-substituted β-carboline ligands that act as metal-based Mcl-1 inhibitors. Complex (I) was identified as a potent and selective Mcl-1 inhibitor with strong in vitro antitumor activity. Mechanistic studies demonstrated that I disrupted Mcl-1-Bax/Bak heterodimerization and induced Bax/Bak-dependent apoptosis. In addn., I significantly (P < 0.001) inhibited tumor growth in vivo, induced tumor necrosis, and extended survival time in an NCI-H460 xenograft model. Furthermore, I showed no apparent toxicity in mice. Together, these findings indicate that I is a copper-based Mcl-1 inhibitor with high efficacy and low toxicity that could be developed for the treatment of Mcl-1-related cancers.

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    Abulwerdi, F.; Liao, C.; Liu, M.; Azmi, A. S.; Aboukameel, A.; Mady, A. S.; Gulappa, T.; Cierpicki, T.; Owens, S.; Zhang, T.; Sun, D.; Stuckey, J. A.; Mohammad, R. M.; Nikolovska-Coleska, Z. A novel small-molecule inhibitor of Mcl-1 blocks pancreatic cancer growth in vitro and in vivo. Mol. Cancer Ther. 2014, 13, 565– 575,  DOI: 10.1158/1535-7163.MCT-12-0767

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    62

    A Novel Small-Molecule Inhibitor of Mcl-1 Blocks Pancreatic Cancer Growth In Vitro and In Vivo

    Abulwerdi, Fardokht; Liao, Chenzhong; Liu, Meilan; Azmi, Asfar S.; Aboukameel, Amro; Mady, Ahmed S. A.; Gulappa, Thippeswamy; Cierpicki, Tomasz; Owens, Scott; Zhang, Tao; Sun, Duxin; Stuckey, Jeanne A.; Mohammad, Ramzi M.; Nikolovska-Coleska, Zaneta

    Molecular Cancer Therapeutics (2014), 13 (3), 565-575CODEN: MCTOCF; ISSN:1535-7163. (American Association for Cancer Research)

    Using a high-throughput screening (HTS) approach, we have identified and validated several small-mol. Mcl-1 inhibitors (SMI). Here, we describe a novel selective Mcl-1 SMI inhibitor, 2 (UMI-77), developed by structure-based chem. modifications of the lead compd. 1 (UMI-59). We have characterized the binding of UMI-77 to Mcl-1 by using complementary biochem., biophys., and computational methods and detd. its antitumor activity against a panel of pancreatic cancer cells and an in vivo xenograft model. UMI-77 binds to the BH3-binding groove of Mcl-1 with Ki of 490 nmol/L, showing selectivity over other members of the antiapoptotic Bcl-2 family. UMI-77 inhibits cell growth and induces apoptosis in pancreatic cancer cells in a time- and dose-dependent manner, accompanied by cytochrome c release and caspase-3 activation. Coimmunopptn. expts. revealed that UMI-77 blocks the heterodimerization of Mcl-1/Bax and Mcl-1/Bak in cells, thus antagonizing the Mcl-1 function. The Bax/Bak-dependent induction of apoptosis was further confirmed using murine embryonic fibroblasts that are Bax- and Bak-deficient. In an in vivo BxPC-3 xenograft model, UMI-77 effectively inhibited tumor growth. Western blot anal. in tumor remnants revealed enhancement of proapoptotic markers and significant decrease of survivin. Collectively, these promising findings show the therapeutic potential of Mcl-1 inhibitors against pancreatic cancer and warrant further preclin. investigations. Mol Cancer Ther; 13(3); 565-75. 2013 AACR.

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63. 63

    Lee, T.; Bian, Z.; Zhao, B.; Hogdal, L. J.; Sensintaffar, J. L.; Goodwin, C. M.; Belmar, J.; Shaw, S.; Tarr, J. C.; Veerasamy, N.; Matulis, S. M.; Koss, B.; Fischer, M. A.; Arnold, A. L.; Camper, D. V.; Browning, C. F.; Rossanese, O. W.; Budhraja, A.; Opferman, J.; Boise, L. H.; Savona, M. R.; Letai, A.; Olejniczak, E. T.; Fesik, S. W. Discovery and biological characterization of potent myeloid cell leukemia-1 inhibitors. FEBS Lett. 2017, 591, 240– 251,  DOI: 10.1002/1873-3468.12497

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    63

    Discovery and biological characterization of potent myeloid cell leukemia-1 inhibitors

    Lee, Taekyu; Bian, Zhiguo; Zhao, Bin; Hogdal, Leah J.; Sensintaffar, John L.; Goodwin, Craig M.; Belmar, Johannes; Shaw, Subrata; Tarr, James C.; Veerasamy, Nagarathanam; Matulis, Shannon M.; Koss, Brian; Fischer, Melissa A.; Arnold, Allison L.; Camper, DeMarco V.; Browning, Carrie F.; Rossanese, Olivia W.; Budhraja, Amit; Opferman, Joseph; Boise, Lawrence H.; Savona, Michael R.; Letai, Anthony; Olejniczak, Edward T.; Fesik, Stephen W.

    FEBS Letters (2017), 591 (1), 240-251CODEN: FEBLAL; ISSN:0014-5793. (Wiley-Blackwell)

    Myeloid cell leukemia 1 (Mcl-1) is an antiapoptotic member of the Bcl-2 family of proteins that when overexpressed is assocd. with high tumor grade, poor survival, and resistance to chemotherapy. Mcl-1 is amplified in many human cancers, and knockdown of Mcl-1 using RNAi can lead to apoptosis. Thus, Mcl-1 is a promising cancer target. Here, the authors describe the discovery of picomolar Mcl-1 inhibitors that cause caspase activation, mitochondrial depolarization, and selective growth inhibition. These compds. represent valuable tools to study the role of Mcl-1 in cancer and serve as useful starting points for the discovery of clin. useful Mcl-1 inhibitors.

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    Lu, X.; Liu, Y. C.; Orvig, C.; Liang, H.; Chen, Z. F. Discovery of β-carboline copper(II) complexes as Mcl-1 inhibitor and in vitro and in vivo activity in cancer models. Eur. J. Med. Chem. 2019, 181, 111567,  DOI: 10.1016/j.ejmech.2019.111567

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    64

    Discovery of β-carboline copper(II) complexes as Mcl-1 inhibitor and in vitro and in vivo activity in cancer models

    Lu, Xing; Liu, Yan-Cheng; Orvig, Chris; Liang, Hong; Chen, Zhen-Feng

    European Journal of Medicinal Chemistry (2019), 181 (), 111567CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    Mcl-1 is an anti-apoptotic member of Bcl-2 family proteins. The development of inhibitors of Mcl-1 has been challenging. To develop metal-based Mcl-1 inhibitors, twenty two copper(II) complexes 25-46 with 9-substituted β-carboline derivs. were reported. Complexes 38 and 39 showed higher cytotoxicity than the corresponding ligands or cisplatin. The most potent complex 39 presented higher selectivity to Mcl-1 than other Bcl-2 family proteins, and killed cancer cells via Bax/Bak mediated apoptosis. Complex 39 showed an excellent safety profile in mouse model, and significantly inhibited the tumor growth in NCI-H460 tumor bearing model, which is more potent than AZD5991 at the same dosage. Complex 39 prolonged the survival time of the tumor bearing mice. Complex 39 is the first metal-based Mcl-1 inhibitor acting as a potential anticancer agent.

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65. 65

    Richard, D. J.; Lena, R.; Bannister, T.; Blake, N.; Pierceall, W. E.; Carlson, N. E.; Keller, C. E.; Koenig, M.; He, Y.; Minond, D.; Mishra, J.; Cameron, M.; Spicer, T.; Hodder, P.; Cardone, M. H. Hydroxyquinoline-derived compounds and analoguing of selective Mcl-1 inhibitors using a functional biomarker. Bioorg. Med. Chem. 2013, 21, 6642– 6649,  DOI: 10.1016/j.bmc.2013.08.017

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    65

    Hydroxyquinoline-derived compounds and analoguing of selective Mcl-1 inhibitors using a functional biomarker

    Richard, David J.; Lena, Ryan; Bannister, Thomas; Blake, Noel; Pierceall, William E.; Carlson, Nicole E.; Keller, Christina Eberhart; Koenig, Marcel; He, Yuanjun; Minond, Dmitriy; Mishra, Jitendra; Cameron, Michael; Spicer, Timothy; Hodder, Peter; Cardone, Michael H.

    Bioorganic & Medicinal Chemistry (2013), 21 (21), 6642-6649CODEN: BMECEP; ISSN:0968-0896. (Elsevier B.V.)

    Anti-apoptotic Bcl-2 family proteins are important oncol. therapeutic targets. To date, BH3 mimetics that abrogate anti-apoptotic activity have largely been directed at Bcl-2 and/or Bcl-xL. One obsd. mechanism of resistance to these inhibitors is increased Mcl-1 levels in cells exposed to such therapeutics. For this reason, and because Mcl-1 is important in the onset of lymphoid, myeloid, and other cancers, it has become a target of great interest. However, small mol. inhibitors displaying potency and selectivity for Mcl-1 are lacking. Identifying such compds. has been challenging due to difficulties in translating the target selectivity obsd. at the biochem. level to the cellular level. Herein we report the results of an HTS strategy coupled with directed hit optimization. Compds. identified have selective Mcl-1 inhibitory activity with greater than 100-fold reduced affinity for Bcl-xL. The selectivity of these compds. at the cellular level was validated using BH3 profiling, a novel personalized diagnostic approach. This assay provides an important functional biomarker that allows for the characterization of cells based upon their dependencies on various anti-apoptotic Bcl-2 proteins. We demonstrate that cells dependent on Mcl-1 or Bcl-2/Bcl-xL for survival are commensurately responsive to compds. that genuinely target those proteins. The identification of compd. 9 with uniquely validated and selective Mcl-1 inhibitory activity provides a valuable tool to those studying the intrinsic apoptosis pathway and highlights an important approach in the development of a first-in-class cancer therapeutic.

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    Petros, A. M.; Swann, S. L.; Song, D.; Swinger, K.; Park, C.; Zhang, H.; Wendt, M. D.; Kunzer, A. R.; Souers, A. J.; Sun, C. Fragment-based discovery of potent inhibitors of the anti-apoptotic MCL-1 protein. Bioorg. Med. Chem. Lett. 2014, 24, 1484– 1488,  DOI: 10.1016/j.bmcl.2014.02.010

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    66

    Fragment-based discovery of potent inhibitors of the anti-apoptotic MCL-1 protein

    Petros, Andrew M.; Swann, Steven L.; Song, Danying; Swinger, Kerren; Park, Chang; Zhang, Haichao; Wendt, Michael D.; Kunzer, Aaron R.; Souers, Andrew J.; Sun, Chaohong

    Bioorganic & Medicinal Chemistry Letters (2014), 24 (6), 1484-1488CODEN: BMCLE8; ISSN:0960-894X. (Elsevier B.V.)

    Apoptosis is regulated by the BCL-2 family of proteins, which is comprised of both pro-death and pro-survival members. Evasion of apoptosis is a hallmark of malignant cells. One way in which cancer cells achieve this evasion is through overexpression of the pro-survival members of the BCL-2 family. Overexpression of MCL-1, a pro-survival protein, has been shown to be a resistance factor for Navitoclax, a potent inhibitor of BCL-2 and BCL-XL. Here we describe the use of fragment screening methods and structural biol. to drive the discovery of novel MCL-1 inhibitors from two distinct structural classes. Specifically, cores derived from a biphenyl sulfonamide and salicylic acid were uncovered in an NMR-based fragment screen and elaborated using high throughput analog synthesis. This culminated in the discovery of selective and potent inhibitors of MCL-1 that may serve as promising leads for medicinal chem. optimization efforts.

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67. 67

    Kotschy, A.; Szlavik, Z.; Murray, J.; Davidson, J.; Maragno, A. L.; Le Toumelin-Braizat, G.; Chanrion, M.; Kelly, G. L.; Gong, J. N.; Moujalled, D. M.; Bruno, A.; Csekei, M.; Paczal, A.; Szabo, Z. B.; Sipos, S.; Radics, G.; Proszenyak, A.; Balint, B.; Ondi, L.; Blasko, G.; Robertson, A.; Surgenor, A.; Dokurno, P.; Chen, I.; Matassova, N.; Smith, J.; Pedder, C.; Graham, C.; Studeny, A.; Lysiak-Auvity, G.; Girard, A. M.; Grave, F.; Segal, D.; Riffkin, C. D.; Pomilio, G.; Galbraith, L. C.; Aubrey, B. J.; Brennan, M. S.; Herold, M. J.; Chang, C.; Guasconi, G.; Cauquil, N.; Melchiore, F.; Guigal-Stephan, N.; Lockhart, B.; Colland, F.; Hickman, J. A.; Roberts, A. W.; Huang, D. C.; Wei, A. H.; Strasser, A.; Lessene, G.; Geneste, O. The MCL1 inhibitor S63845 is tolerable and effective in diverse cancer models. Nature 2016, 538, 477– 482,  DOI: 10.1038/nature19830

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    67

    The MCL1 inhibitor S63845 is tolerable and effective in diverse cancer models

    Kotschy Andras; Szlavik Zoltan; Csekei Marton; Paczal Attila; Szabo Zoltan B; Sipos Szabolcs; Radics Gabor; Proszenyak Agnes; Balint Balazs; Ondi Levente; Blasko Gabor; Murray James; Davidson James; Robertson Alan; Surgenor Allan; Dokurno Pawel; Chen Ijen; Matassova Natalia; Smith Julia; Pedder Christopher; Graham Christopher; Maragno Ana Leticia; Le Toumelin-Braizat Gaetane; Chanrion Maia; Bruno Alain; Studeny Aurelie; Lysiak-Auvity Gaelle; Girard Anne-Marie; Grave Fabienne; Guasconi Ghislaine; Cauquil Nicolas; Colland Frederic; Hickman John A; Geneste Olivier; Kelly Gemma L; Gong Jia-Nan; Segal David; Riffkin Chris D; Galbraith Laura C A; Aubrey Brandon J; Brennan Margs S; Herold Marco J; Chang Catherine; Roberts Andrew W; Huang David C S; Strasser Andreas; Lessene Guillaume; Kelly Gemma L; Gong Jia-Nan; Segal David; Riffkin Chris D; Galbraith Laura C A; Aubrey Brandon J; Brennan Margs S; Herold Marco J; Chang Catherine; Roberts Andrew W; Huang David C S; Strasser Andreas; Lessene Guillaume; Moujalled Donia M; Pomilio Giovanna; Wei Andrew H; Aubrey Brandon J; Roberts Andrew W; Melchiore Fabien; Guigal-Stephan Nolwen; Lockhart Brian; Roberts Andrew W; Wei Andrew H; Lessene Guillaume

    Nature (2016), 538 (7626), 477-482 ISSN:.

    Avoidance of apoptosis is critical for the development and sustained growth of tumours. The pro-survival protein myeloid cell leukemia 1 (MCL1) is overexpressed in many cancers, but the development of small molecules targeting this protein that are amenable for clinical testing has been challenging. Here we describe S63845, a small molecule that specifically binds with high affinity to the BH3-binding groove of MCL1. Our mechanistic studies demonstrate that S63845 potently kills MCL1-dependent cancer cells, including multiple myeloma, leukaemia and lymphoma cells, by activating the BAX/BAK-dependent mitochondrial apoptotic pathway. In vivo, S63845 shows potent anti-tumour activity with an acceptable safety margin as a single agent in several cancers. Moreover, MCL1 inhibition, either alone or in combination with other anti-cancer drugs, proved effective against several solid cancer-derived cell lines. These results point towards MCL1 as a target for the treatment of a wide range of tumours.

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68. 68

    Szlavik, Z.; Csekei, M.; Paczal, A.; Szabo, Z. B.; Sipos, S.; Radics, G.; Proszenyak, A.; Balint, B.; Murray, J.; Davidson, J.; Chen, I.; Dokurno, P.; Surgenor, A. E.; Daniels, Z. M.; Hubbard, R. E.; Le Toumelin-Braizat, G.; Claperon, A.; Lysiak-Auvity, G.; Girard, A. M.; Bruno, A.; Chanrion, M.; Colland, F.; Maragno, A. L.; Demarles, D.; Geneste, O.; Kotschy, A. Discovery of S64315, a potent and selective Mcl-1 inhibitor. J. Med. Chem. 2020, 63, 13762– 13795,  DOI: 10.1021/acs.jmedchem.0c01234

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    Discovery of S64315, a Potent and Selective Mcl-1 Inhibitor

    Szlavik, Zoltan; Csekei, Marton; Paczal, Attila; Szabo, Zoltan B.; Sipos, Szabolcs; Radics, Gabor; Proszenyak, Agnes; Balint, Balazs; Murray, James; Davidson, James; Chen, Ijen; Dokurno, Pawel; Surgenor, Allan E.; Daniels, Zoe Marie; Hubbard, Roderick E.; Le Toumelin-Braizat, Gaetane; Claperon, Audrey; Lysiak-Auvity, Gaelle; Girard, Anne-Marie; Bruno, Alain; Chanrion, Maia; Colland, Frederic; Maragno, Ana-Leticia; Demarles, Didier; Geneste, Olivier; Kotschy, Andras

    Journal of Medicinal Chemistry (2020), 63 (22), 13762-13795CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (Mcl-1) has emerged as an attractive target for cancer therapy. It is an antiapoptotic member of the Bcl-2 family of proteins, whose upregulation in human cancers is assocd. with high tumor grade, poor survival, and resistance to chemotherapy. Here we report the discovery of our clin. candidate S64315, a selective small mol. inhibitor of Mcl-1. Starting from a fragment derived lead compd., we have conducted structure guided optimization that has led to a significant (3 log) improvement of target affinity as well as cellular potency. The presence of hindered rotation along a biaryl axis has conferred high selectivity to the compds. against other members of the Bcl-2 family. During optimization, we have also established predictive PD markers of Mcl-1 inhibition and achieved both efficient in vitro cell killing and tumor regression in Mcl-1 dependent cancer models. The preclin. candidate has drug-like properties that have enabled its development and entry into clin. trials.

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69. 69

    Zhu, P. J.; Yu, Z. Z.; You, Q. D.; Jiang, Z. Y. Myeloid cell leukemin-1 inhibitors: a growing arsenal for cancer therapy. Drug Discovery Today 2020, 25, 1873– 1882,  DOI: 10.1016/j.drudis.2020.07.021

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    69

    Myeloid cell leukemin-1 inhibitors and a growing arsenal for cancer therapy

    Zhu, Peng-Ju; Yu, Ze-Zhou; You, Qi-Dong; Jiang, Zheng-Yu

    Drug Discovery Today (2020), 25 (10), 1873-1882CODEN: DDTOFS; ISSN:1359-6446. (Elsevier Ltd.)

    A Review. B-cell lymphoma-2 (Bcl-2) family proteins, comprising proapoptotic proteins (Bax and Bak), antiapoptotic proteins (Bcl-2, Bcl-XL, Bcl-w, Mcl-1, and A1) and BCL-2 homol. domain 3 (BH3)-only proteins (Bid, Noxa, and Puma), have long been identified as pivotal apoptosis regulators. As an antiapoptotic member, myeloid cell leukemin-1 (Mcl-1) can bind with proapoptotic proteins and inhibit apoptosis. Mcl-1 is frequently overexpressed and closely assocd. with oncogenesis and poor prognosis in several cancers, posing a tremendous obstacle for cancer therapy. Recently, an increasing no. of Mcl-1-selective small-mol. inhibitors have entered preclin. studies and advanced into clin. trials. In this review, we briefly introduce the role of Mcl-1 in apoptosis and highlight the recent development of Mcl-1 small-mol. inhibitors.

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70. 70

    Li, X.; Dou, J.; You, Q.; Jiang, Z. Inhibitors of BCL2A1/Bfl-1 protein: Potential stock in cancer therapy. Eur. J. Med. Chem. 2021, 220, 113539,  DOI: 10.1016/j.ejmech.2021.113539

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    70

    Inhibitors of BCL2A1/Bfl-1 protein: Potential stock in cancer therapy

    Li, Xue; Dou, Junwei; You, Qidong; Jiang, Zhengyu

    European Journal of Medicinal Chemistry (2021), 220 (), 113539CODEN: EJMCA5; ISSN:0223-5234. (Elsevier Masson SAS)

    The Bcl-2 family members rigorously regulate cell endogenous apoptosis, and targeting anti-apoptotic members is a hot topic in design of anti-cancer drugs. At present, FDA and EMA have approved Bcl-2 inhibitor Venetoclax (ABT-199) for treating chronic lymphocytic leukemia (CLL). However, inhibitors of anti-apoptotic protein BCL2A1/Bfl-1 have not been vigorously developed, and no mol. with ideal activity and selectivity has been found yet. Here we review the biol. function and protein structure of Bfl-1, discuss the therapeutic potential and list the currently reported inhibitory peptides and small mols. This will provide a ref. for Bfl-1 targeting drug discovery in the future.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BB3MXhtFGlt7zE&md5=cd2472d31fd571818796cbd209ad63e2
71. 71

    Chang, J.; Wang, Y.; Shao, L.; Laberge, R. M.; Demaria, M.; Campisi, J.; Janakiraman, K.; Sharpless, N. E.; Ding, S.; Feng, W.; Luo, Y.; Wang, X.; Aykin-Burns, N.; Krager, K.; Ponnappan, U.; Hauer-Jensen, M.; Meng, A.; Zhou, D. Clearance of senescent cells by ABT263 rejuvenates aged hematopoietic stem cells in mice. Nat. Med. 2016, 22, 78– 83,  DOI: 10.1038/nm.4010

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    71

    Clearance of senescent cells by ABT263 rejuvenates aged hematopoietic stem cells in mice

    Chang, Jianhui; Wang, Yingying; Shao, Lijian; Laberge, Remi-Martin; Demaria, Marco; Campisi, Judith; Janakiraman, Krishnamurthy; Sharpless, Norman E.; Ding, Sheng; Feng, Wei; Luo, Yi; Wang, Xiaoyan; Aykin-Burns, Nukhet; Krager, Kimberly; Ponnappan, Usha; Hauer-Jensen, Martin; Meng, Aimin; Zhou, Daohong

    Nature Medicine (New York, NY, United States) (2016), 22 (1), 78-83CODEN: NAMEFI; ISSN:1078-8956. (Nature Publishing Group)

    Senescent cells (SCs) accumulate with age and after genotoxic stress, such as total-body irradn. (TBI). Clearance of SCs in a progeroid mouse model using a transgenic approach delays several age-assocd. disorders, suggesting that SCs play a causative role in certain age-related pathologies. Thus, a 'senolytic' pharmacol. agent that can selectively kill SCs holds promise for rejuvenating tissue stem cells and extending health span. To test this idea, we screened a collection of compds. and identified ABT263 (a specific inhibitor of the anti-apoptotic proteins BCL-2 and BCL-xL) as a potent senolytic drug. We show that ABT263 selectively kills SCs in culture in a cell type- and species-independent manner by inducing apoptosis. Oral administration of ABT263 to either sublethally irradiated or normally aged mice effectively depleted SCs, including senescent bone marrow hematopoietic stem cells (HSCs) and senescent muscle stem cells (MuSCs). Notably, this depletion mitigated TBI-induced premature aging of the hematopoietic system and rejuvenated the aged HSCs and MuSCs in normally aged mice. Our results demonstrate that selective clearance of SCs by a pharmacol. agent is beneficial in part through its rejuvenation of aged tissue stem cells. Thus, senolytic drugs may represent a new class of radiation mitigators and anti-aging agents.

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72. 72

    Munkhbaatar, E.; Dietzen, M.; Agrawal, D.; Anton, M.; Jesinghaus, M.; Boxberg, M.; Pfarr, N.; Bidola, P.; Uhrig, S.; Höckendorf, U.; Meinhardt, A. L.; Wahida, A.; Heid, I.; Braren, R.; Mishra, R.; Warth, A.; Muley, T.; Poh, P. S. P.; Wang, X.; Fröhling, S.; Steiger, K.; Slotta-Huspenina, J.; van Griensven, M.; Pfeiffer, F.; Lange, S.; Rad, R.; Spella, M.; Stathopoulos, G. T.; Ruland, J.; Bassermann, F.; Weichert, W.; Strasser, A.; Branca, C.; Heikenwalder, M.; Swanton, C.; McGranahan, N.; Jost, P. J. MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically. Nat. Commun. 2020, 11, 4527,  DOI: 10.1038/s41467-020-18372-1

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    72

    MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically

    Munkhbaatar, Enkhtsetseg; Dietzen, Michelle; Agrawal, Deepti; Anton, Martina; Jesinghaus, Moritz; Boxberg, Melanie; Pfarr, Nicole; Bidola, Pidassa; Uhrig, Sebastian; Hoeckendorf, Ulrike; Meinhardt, Anna-Lena; Wahida, Adam; Heid, Irina; Braren, Rickmer; Mishra, Ritu; Warth, Arne; Muley, Thomas; Poh, Patrina S. P.; Wang, Xin; Froehling, Stefan; Steiger, Katja; Slotta-Huspenina, Julia; van Griensven, Martijn; Pfeiffer, Franz; Lange, Sebastian; Rad, Roland; Spella, Magda; Stathopoulos, Georgios T.; Ruland, Juergen; Bassermann, Florian; Weichert, Wilko; Strasser, Andreas; Branca, Caterina; Heikenwalder, Mathias; Swanton, Charles; McGranahan, Nicholas; Jost, Philipp J.

    Nature Communications (2020), 11 (1), 4527CODEN: NCAOBW; ISSN:2041-1723. (Nature Research)

    Evasion of programmed cell death represents a crit. form of oncogene addiction in cancer cells. Understanding the mol. mechanisms underpinning cancer cell survival despite the oncogenic stress could provide a mol. basis for potential therapeutic interventions. Here we explore the role of pro-survival genes in cancer cell integrity during clonal evolution in non-small cell lung cancer (NSCLC). We identify gains of MCL-1 at high frequency in multiple independent NSCLC cohorts, occurring both clonally and subclonally. Clonal loss of functional TP53 is significantly assocd. with subclonal gains of MCL-1. In mice, tumor progression is delayed upon pharmacol. or genetic inhibition of MCL-1. These findings reveal that MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BB3cXhvFSitbjE&md5=ca1e26757966980a2bab01fc82448788
73. 73

    Liu, J.; Fang, Z.; Zhang, Q.; Liu, Q.; Bi, X. Silver-catalyzed isocyanide-alkyne cycloaddition: a general and practical method to oligosubstituted pyrroles. Angew. Chem. Int. Ed. Engl. 2013, 52, 6953– 6957,  DOI: 10.1002/anie.201302024

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    Silver-catalyzed isocyanide-alkyne cycloaddition: a general and practical method to oligosubstituted pyrroles

    Liu Jianquan; Fang Zhongxue; Zhang Qian; Liu Qun; Bi Xihe

    Angewandte Chemie (International ed. in English) (2013), 52 (27), 6953-7 ISSN:.

    There is no expanded citation for this reference.

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74. 74

    Kattamuri, P. V.; Yin, J.; Siriwongsup, S.; Kwon, D. H.; Ess, D. H.; Li, Q.; Li, G.; Yousufuddin, M.; Richardson, P. F.; Sutton, S. C.; Kürti, L. Practical singly and doubly electrophilic aminating agents: a new, more sustainable platform for carbon-nitrogen bond formation. J. Am. Chem. Soc. 2017, 139, 11184– 11196,  DOI: 10.1021/jacs.7b05279

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    Practical Singly and Doubly Electrophilic Aminating Agents: A New, More Sustainable Platform for Carbon-Nitrogen Bond Formation

    Kattamuri, Padmanabha V.; Yin, Jun; Siriwongsup, Surached; Kwon, Doo-Hyun; Ess, Daniel H.; Li, Qun; Li, Guigen; Yousufuddin, Muhammed; Richardson, Paul F.; Sutton, Scott C.; Kurti, Laszlo

    Journal of the American Chemical Society (2017), 139 (32), 11184-11196CODEN: JACSAT; ISSN:0002-7863. (American Chemical Society)

    Given the importance of amines in a large no. of biol. active natural products, active pharmaceutical ingredients, agrochems., and functional materials, the development of efficient C-N bond-forming methods with wide substrate scope continues to be at the frontier of research in synthetic org. chem. Here, authors present a general and fundamentally new synthetic approach for the direct, transition-metal-free prepn. of sym. and unsym. diaryl-, arylalkyl-, and dialkylamines that relies on the facile single or double addn. of readily available C-nucleophiles to the nitrogen atom of bench-stable electrophilic aminating agents. Practical single and double polarity reversal (i.e., umpolung) of the nitrogen atom is achieved using sterically and electronically tunable ketomalonate-derived imines and oximes. Overall, this novel approach represents an operationally simple, scalable, and environmentally friendly alternative to transition-metal-catalyzed C-N cross-coupling methods that are currently used to access structurally diverse secondary amines.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BC2sXhtVCkt7jP&md5=38f07ddb4a79a3a4fecdcc40520c0d7c
75. 75

    Cohen, N. A.; Stewart, M. L.; Gavathiotis, E.; Tepper, J. L.; Bruekner, S. R.; Koss, B.; Opferman, J. T.; Walensky, L. D. A competitive stapled peptide screen identifies a selective small molecule that overcomes MCL-1-dependent leukemia cell survival. Chem. Biol. 2012, 19, 1175– 1186,  DOI: 10.1016/j.chembiol.2012.07.018

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    A Competitive Stapled Peptide Screen Identifies a Selective Small Molecule that Overcomes MCL-1-Dependent Leukemia Cell Survival

    Cohen, Nicole A.; Stewart, Michelle L.; Gavathiotis, Evripidis; Tepper, Jared L.; Bruekner, Susanne R.; Koss, Brian; Opferman, Joseph T.; Walensky, Loren D.

    Chemistry & Biology (Oxford, United Kingdom) (2012), 19 (9), 1175-1186CODEN: CBOLE2; ISSN:1074-5521. (Elsevier Ltd.)

    Cancer cells hijack BCL-2 family survival proteins to suppress the death effectors and thereby enforce an immortal state. This is accomplished biochem. by an antiapoptotic surface groove that neutralizes the proapoptotic BH3 α helix of death proteins. Antiapoptotic MCL-1 in particular has emerged as a ubiquitous resistance factor in cancer. Although targeting the BCL-2 antiapoptotic subclass effectively restores the death pathway in BCL-2-dependent cancer, the development of mols. tailored to the binding specificity of MCL-1 has lagged. We previously discovered that a hydrocarbon-stapled MCL-1 BH3 helix is an exquisitely selective MCL-1 antagonist. By deploying this unique reagent in a competitive screen, we identified an MCL-1 inhibitor mol. that selectively targets the BH3-binding groove of MCL-1, neutralizes its biochem. lock-hold on apoptosis, and induces caspase activation and leukemia cell death in the specific context of MCL-1 dependence.

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76. 76

    Kump, K. J.; Miao, L.; Mady, A. S. A.; Ansari, N. H.; Shrestha, U. K.; Yang, Y.; Pal, M.; Liao, C.; Perdih, A.; Abulwerdi, F. A.; Chinnaswamy, K.; Meagher, J. L.; Carlson, J. M.; Khanna, M.; Stuckey, J. A.; Nikolovska-Coleska, Z. Discovery and characterization of 2,5-substituted benzoic acid dual inhibitors of the anti-apoptotic Mcl-1 and Bfl-1 proteins. J. Med. Chem. 2020, 63, 2489– 2510,  DOI: 10.1021/acs.jmedchem.9b01442

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    76

    Discovery and Characterization of 2,5-Substituted Benzoic Acid Dual Inhibitors of the Anti-apoptotic Mcl-1 and Bfl-1 Proteins

    Kump, Karson J.; Miao, Lei; Mady, Ahmed S. A.; Ansari, Nurul H.; Shrestha, Uttar K.; Yang, Yuting; Pal, Mohan; Liao, Chenzhong; Perdih, Andrej; Abulwerdi, Fardokht A.; Chinnaswamy, Krishnapriya; Meagher, Jennifer L.; Carlson, Jacob M.; Khanna, May; Stuckey, Jeanne A.; Nikolovska-Coleska, Zaneta

    Journal of Medicinal Chemistry (2020), 63 (5), 2489-2510CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Anti-apoptotic Bcl-2 family proteins are overexpressed in a wide spectrum of cancers and have become well validated therapeutic targets. Cancer cells display survival dependence on individual or subsets of anti-apoptotic proteins that could be effectively targeted by multimodal inhibitors. We designed a 2,5-substituted benzoic acid scaffold that displayed equipotent binding to Mcl-1 and Bfl-1. Structure-based design was guided by several solved cocrystal structures with Mcl-1, leading to the development of compd. 24, which binds both Mcl-1 and Bfl-1 with Ki values of 100 nM and shows appreciable selectivity over Bcl-2/Bcl-xL. The selective binding profile of 24 was translated to on-target cellular activity in model lymphoma cell lines. These studies lay a foundation for developing more advanced dual Mcl-1/Bfl-1 inhibitors that have potential to provide greater single agent efficacy and broader coverage to combat resistance in several types of cancer than selective Mcl-1 inhibitors alone.

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77. 77

    Bernardo, P. H.; Sivaraman, T.; Wan, K.-F.; Xu, J.; Krishnamoorthy, J.; Song, C. M.; Tian, L.; Chin, J. S. F.; Lim, D. S. W.; Mok, H. Y. K.; Yu, V. C.; Tong, J. C.; Chai, C. L. Structural insights into the design of small molecule inhibitors that selectively antagonize Mcl-1. J. Med. Chem. 2010, 53, 2314– 2318,  DOI: 10.1021/jm901469p

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    77

    Structural Insights into the Design of Small Molecule Inhibitors That Selectively Antagonize Mcl-1

    Bernardo, Paul H.; Sivaraman, Thirunavukkarasu; Wan, Kah-Fei; Xu, Jin; Krishnamoorthy, Janarthanan; Song, Chun Meng; Tian, Liming; Chin, Jasmine S. F.; Lim, Diane S. W.; Mok, Henry Y. K.; Yu, Victor C.; Tong, Joo Chuan; Chai, Christina L. L.

    Journal of Medicinal Chemistry (2010), 53 (5), 2314-2318CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    The screening of a small focused library of rhodanine derivs. as inhibitors of Bcl-2 proteins led to the discovery of two structurally related compds. with different binding profiles against the Bcl-XL and the Mcl-1 proteins. Subsequent NMR studies with mutant proteins and in silico docking studies provide a possible rationale for the obsd. specificity.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BC3cXhvF2ktbg%253D&md5=c033784e92b321c2455a5d8b7594d5f6
78. 78

    Szlavik, Z.; Ondi, L.; Csekei, M.; Paczal, A.; Szabo, Z. B.; Radics, G.; Murray, J.; Davidson, J.; Chen, I.; Davis, B.; Hubbard, R. E.; Pedder, C.; Dokurno, P.; Surgenor, A.; Smith, J.; Robertson, A.; LeToumelin-Braizat, G.; Cauquil, N.; Zarka, M.; Demarles, D.; Perron-Sierra, F.; Claperon, A.; Colland, F.; Geneste, O.; Kotschy, A. Structure-guided discovery of a selective Mcl-1 inhibitor with cellular activity. J. Med. Chem. 2019, 62, 6913– 6924,  DOI: 10.1021/acs.jmedchem.9b00134

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    78

    Structure-Guided Discovery of a Selective Mcl-1 Inhibitor with Cellular Activity

    Szlavik, Zoltan; Ondi, Levente; Csekei, Marton; Paczal, Attila; Szabo, Zoltan B.; Radics, Gabor; Murray, James; Davidson, James; Chen, Ijen; Davis, Ben; Hubbard, Roderick E.; Pedder, Christopher; Dokurno, Pawel; Surgenor, Allan; Smith, Julia; Robertson, Alan; LeToumelin-Braizat, Gaetane; Cauquil, Nicolas; Zarka, Marion; Demarles, Didier; Perron-Sierra, Francoise; Claperon, Audrey; Colland, Frederic; Geneste, Olivier; Kotschy, Andras

    Journal of Medicinal Chemistry (2019), 62 (15), 6913-6924CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    Myeloid cell leukemia 1 (Mcl-1), an antiapoptotic member of the Bcl-2 family of proteins, whose upregulation when obsd. in human cancers is assocd. with high tumor grade, poor survival, and resistance to chemotherapy, has emerged as an attractive target for cancer therapy. Here, we report the discovery of selective small mol. inhibitors of Mcl-1 that inhibit cellular activity. Fragment screening identified thienopyrimidine amino acids as promising but nonselective hits that were optimized using NMR and X-ray-derived structural information. The introduction of hindered rotation along a biaryl axis has conferred high selectivity to the compds., and cellular activity was brought on scale by offsetting the neg. charge of the anchoring carboxylate group. The obtained compds. described here exhibit nanomolar binding affinity and mechanism-based cellular efficacy, caspase induction, and growth inhibition. These early research efforts illustrate drug discovery optimization from thienopyrimidine hits to a lead compd., the chem. series leading to the identification of our more advanced compds. S63845 and S64315.

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    https://chemport.cas.org/services/resolver?origin=ACS&resolution=options&coi=1%3ACAS%3A528%3ADC%252BC1MXht1ensrvN&md5=e94a3a9ac96f5693406cafa185484470
79. 79

    Wu, Y.; Jiang, Z.; Li, Z.; Gu, J.; You, Q.; Zhang, X. Click chemistry-based discovery of [3-hydroxy-5-(1h-1,2,3-triazol-4-yl)picolinoyl]glycines as orally active hypoxia-inducing factor prolyl hydroxylase inhibitors with favorable safety profiles for the treatment of anemia. J. Med. Chem. 2018, 61, 5332– 5349,  DOI: 10.1021/acs.jmedchem.8b00549

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    Click Chemistry-Based Discovery of [3-Hydroxy-5-(1H-1,2,3-triazol-4-yl)picolinoyl]glycines as Orally Active Hypoxia-Inducing Factor Prolyl Hydroxylase Inhibitors with Favorable Safety Profiles for the Treatment of Anemia

    Wu, Yue; Jiang, Zhensheng; Li, Zhihong; Gu, Jing; You, Qidong; Zhang, Xiaojin

    Journal of Medicinal Chemistry (2018), 61 (12), 5332-5349CODEN: JMCMAR; ISSN:0022-2623. (American Chemical Society)

    As a gene assocd. with anemia, the erythropoiesis gene is physiol. expressed under hypoxia regulated by †hypoxia-inducing factor-α (HIF-α). Thus, stabilizing HIF-α is a potent strategy to stimulate the expression and secretion of erythropoiesis. In this study, we applied click chem. to the discovery of HIF prolyl hydroxylase 2 (HIF-PHD2) inhibitors for the first time, and a series of triazole compds. showed preferable inhibitory activity in fluorescence polarization assays. Of particular note was the orally active HIF-PHD inhibitor 15i (IC50 = 62.23 nM), which was almost ten times more active than the phase III drug FG-4592 (IC50 = 591.4 nM). Furthermore, it can upregulate the Hb of cisplatin-induced anemia mice (120 g/L) to normal levels (160 g/L) with no apparent toxicity obsd. in vivo. These results confirm that triazole compd. 15i is a promising candidate for the treatment of renal anemia.

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